- Email: [email protected]
Berberine pharmacology and the gut microbiota: A hidden therapeutic link
Journal Pre-proof Berberine Pharmacology and the Gut Microbiota: A Hidden Therapeutic Link Solomon Habtemariam
PII:
S1043-6618(20)30149-3
DOI:
https://doi.org/10.1016/j.phrs.2020.104722
Reference:
YPHRS 104722
To appear in:
Pharmacological Research
Received Date:
13 January 2020
Revised Date:
21 February 2020
Accepted Date:
23 February 2020
Please cite this article as: Habtemariam S, Berberine Pharmacology and the Gut Microbiota: A Hidden Therapeutic Link, Pharmacological Research (2020), doi: https://doi.org/10.1016/j.phrs.2020.104722
This is a PDF file of an article that has undergone enhancements after acceptance, such as the addition of a cover page and metadata, and formatting for readability, but it is not yet the definitive version of record. This version will undergo additional copyediting, typesetting and review before it is published in its final form, but we are providing this version to give early visibility of the article. Please note that, during the production process, errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain. © 2020 Published by Elsevier.
Berberine Pharmacology and the Gut Microbiota: A Hidden Therapeutic Link Solomon Habtemariam Pharmacognosy Research Laboratories & Herbal Analysis Services UK, University of Greenwich, ChathamMaritime, Kent ME4 4TB, UK; [email protected]; Tel.: +44-208-331-8302 Received: 26 November 2019; Accepted: 11 December 2019; Published: date
re
-p
ro of
Graphical abstract
Abstract
Jo
ur
na
lP
Berberine is a natural pentacyclic isoquinoline alkaloid that has been isolated as the principal component of many popular medicinal plants such as the genus Berberis, Coptis and Hydrastis. The multifunctional nature of berberine as a therapeutic agent is an attribute of its diverse effects on enzymes, receptors and cell signalling pathways. Through specific and general antioxidant and antiinflammatory mechanisms, its polypharmacology has been established. Intriguingly, this is despite the poor bioavailability of berberine in animal models and hence begging the question how it induces its reputed effects in vivo. A growing evidence now suggest the role of the gut microbiota, the so-called the hidden organ, as targets for the multifunctional role of berberine. Evidences are herein scrutinised to show that the structural and numerical changes in the gut microbiota under pathological conditions are reversed by berberine. Examples in the pharmacokinetics field, obesity, hyperlipidaemia, diabetes, cancer, inflammatory disease conditions, etc. are used to show the link between the gut microbiota and the polypharmacology of berberine. Keywords: Berberine, microbiota, diabetes, obesity, hyperlipidaemia, infection, inflammation, SCFA, Firmicutes-to-Bacteroidetes ratio.
1. Introduction
-p
ro of
Berberine (Figure 1) is a natural pentacyclic isoquinoline alkaloid which is abundantly found as a principal constituent of many medicinal plants. The classic examples of berberine sources are the stems and roots of Berberis species including B. aristata [1,2], B. darwinii [3,4], B. Petiolaris [5] and B. vulgaris [6]. These berberine-containing plants with high yield of up to 5% of their dry weight have been reported. Composition up to 8-9% berberine in the rhizomes of many medicinal plants have also been known with the most researched plants to date include Argemone mexicana, Coptis chinensis (Chinese goldthread), C. japonica, C. teeta, Eschscholzia californica and Hydrastis Canadensis or goldenseal, Mahonia aquifolium, Tinospora cordifolia, Xanthorhiza simplicissima, and Phellodendron amurense. One characteristic feature of berberine is its distinctive yellowish colour that gives the source plant materials their yellow to gold appearance (Figure 1).
re
Figure 1. The structure of berberine and its deep yellow colour.
Jo
ur
na
lP
In its chemically pure form, berberine is known to be first isolated from H. canadensis (goldenseal) in 1917 [7] but its use as a principal component of plants was dated to antiquity primarily as a dye (e.g., the textile industry) due to its deep yellow and yellow fluorescent characteristics. Its medicinal use was also dated for centuries as an active principle for numerous medicinal plants which are still in use to date including as ingredients of various food supplements. The pharmacology of berberine has been extensively studied and include anti-inflammatory [8,9], anticancer [10-12], antidiabetic [13-15], antiobesity and anti-hyperlipidaemic [14,16], cardioprotective [17,18] and spatial memory enhancement [19-21] effects. The plethora of pharmacological effects recorded for berberine attributes to some specific effects on enzymes, receptors and other biological targets along with other general effects such as antioxidant and anti-inflammatory properties. As with many natural products, the therapeutic potential of berberine could be explained by the polypharmacology principle of drug action [22] though research on the mechanisms of action that account to its diverse effects still continues. This article is designed to shade some light on the potential contribution of the gut microbiota to berberine’s multifunctional bioactivity.
2. Pharmacokinetics Even though berberine is a cationic alkaloid, its structure is by no means optimised for rapid absorption from the gut. It is sparingly soluble in water implying that it has poor intestinal absorption and/or bioavailability. In fact, the absolute bioavailability of berberine is far less than 1% given that even the absorbed berberine from the gut could be excreted back to the intestinal lumen through the action of P-glycoprotein. Chen et al. [23] reported absolute bioavailability from the oral route in rats as 0.68%, and as expected, inhibitors of P-glycoprotein could increase bioavailability from the intestine. Berberine absorption in rats could also be improved by up to 6-times by P-glycoprotein inhibitors
Jo
ur
na
lP
re
-p
ro of
suggesting the contribution of P-glycoprotein to the poor intestinal absorption of berberine [24]. An absolute oral bioavailability in rats of 0.36% has also been reported making intestinal first-pass elimination of berberine as the major barrier to its oral bioavailability [25]. With such poor degree of absorption from the gut, berberine ingested in hamsters is largely accumulated in the gut (not the circulation) and its bioavailability through intraperitoneal route is much better than the oral/intragastric route [26]. Based on HPLC analysis of human plasma following berberine oral dose, the absolute bioavailability was considered extremely low with the maximum plasma concentration of about 0.4 ng/ml obtained following 400 mg oral dose [27]. Despite all these, berberine has been shown to induce pharmacological effects in a plethora of animal models. Once absorbed, berberine has also shown to be distributed into all major organs with the highest amount obtained in the liver and readily excreted via the urine [28]. One of the emerging links between the expected poor bioavailability of berberine and its pharmacology is the gut microbiota that modulate both the pharmacokinetics profile and its biological effects. In beagle dogs, for example, oral administration of berberine leads to changes in the intestinal bacterial composition and butyrate (a product of bacteria) level in the gut [29]. In this case, treatment with berberine for seven days could increase the abundance of butyrate- and the nitroreductases-producing bacteria though the plasma level of berberine was still very low with the maximum level detected following an oral administration of 50 mg/kg was 37 ng/ml [29]. Earlier studies have also shown that berberine could enhance the oral bioavailability of other drugs. The bioavailability of ciclosporin A, for example, was shown to be augmented in healthy human volunteers resulting from the suspected decrease in liver and intestinal metabolism through inhibition of CYP3A4 [30]. Recent studies however pinpoint the role of the gut microbiota as a major target for modulation of drug pharmacokinetics by berberine. Accordingly, the pharmacokinetics interaction of berberine and metformin include the berberine-induced increase in metformin level coupled with decreased metformin degradation by rat and human intestinal bacteria [31]. Guo et al. [32] further showed that oral administration of berberine in mice could lead to increased expression of bile acidssynthetic enzymes (Cyp7a1 and 8b1) and uptake transporter (Ntcp) in the liver while the level of Bacteroides in the terminal ileum and large bowel were enhanced. An inspiring research on the role of the gut microbiota in the pharmacokinetics of berberine and potential variations between Chinese and Africans has been investigated by Alioga et al. [33]. The study revealed a higher abundance of the genera Prevotella, Bacteroides, and Megamonas (34.22, 13.88, and 10.68%, respectively) in the Chinese than the Africans subjects with more extensive metabolism was observed in the Chinese group. This study highlights that inter-individual and inter-racial differences in drug metabolism could be linked to variations in the gut microbiota. Dietary habits and antibiotics therapy are also likely to affect the state of the individual’s response in the pharmacokinetics and pharmacology of berberine. One mechanism for enhancing the biological activity of berberine by the gut microbiota lies in their ability to convert it into a better absorbable form, dihydroberberine. Feng et al. [34] reported a 5-fold increase in intestinal absorption rate for dihydroberberine than berberine in animals. In mice, the microbiota could reduce berberine to dihydroberberine which is absorbed into intestinal tissue and subsequently oxidised back to berberine to enter the blood stream. This process too could be ameliorated by treatment with antibiotics [34]. The dual effect of berberine in its pharmacology either by enhancing the gut microbiota or through its own specific mechanism of action was noted by the study of Wang et al. [35]. They have shown that some of the effect of berberine could be attributed to the increased butyrate production in the gut and increased abundance of such bacteria which has profound effect on blood lipid and glucose levels. The mechanism of butyrate itself on blood level of glucose and lipids was however different begging into a question of multiple mechanisms of action. The role of the gut microbiota as mediators of berberine’s polypharmacology is detailed further in the following sections. 3.
General effect on the gut microbiota
re
-p
ro of
Although the direct antibacterial effect of berberine in vitro is somehow weak, the compound is widely known as an antibacterial agent including in vivo. Not surprisingly, one of its known mechanism in ameliorating intestinal inflammation in humans is through direct antibacterial action [36]. This includes effects against Escherichia coli in vitro [37,38]; Clostridium difficile-induced intestinal injury model in mice [39] and anti-diarrhoeal effect in human [40]. The most important function of berberine related to the present communication is its ability to modify the composition of the gut microbiota. Earlier studies have shown that berberine can induce cell death in harmful gut bacteria while enhancing the composition of beneficial bacteria including Bifidobacterium adolescentis and Lactobacillus acidophilus [41,42]. The mechanism of berberine in modifying diseases is thus somehow similar with those of probiotics [43-46]. Hence, under disease conditions such as colitis, inflammatory bowel disease (IBD) or related pathologies associated with gut inflammation, berberine can reverse the increased prevalence of harmful bacteria such as E. coli and enterococci bacteria and the pathology-induced decreased Lactobacilli and Bifidobacteria. The mild diarrhoea induction under clinical condition by berberine is also shown to be coupled with gut microbiota dysbiosis such as increased abundances of the families Porphyromonadaceae and Prevotellaceae as well as the genera of Parabacteroides, Prevotellaceae_UCG-001 and Prevotellaceae_NK3B31_group [47]. Analysis of microbiota in the gut of broilers under high stocking density has further shown that treatment with berberine could lower the level of E. coli while increasing Lactobacillus in the cecum [48]. Most of the experiments conducted on berberine discussed in the following sections are based on changes on the profile of the gut microbiota population. While the composition of the human gut microbiota could change with diet and many other factors, studies on the bacterial 16S rRNA gene sequences from the faecal microbiota of humans and 59 other mammalian species have shown the prevalent groups as Firmicutes (65.7%) and to the Bacteroidetes (16.3%) and small proportion of Proteobacteria (8.8%), Actinobacteria (4.7%), Verrucomicrobia (2.2%), Fusobacteria (0.67%), and others [49]. The composition of these gut microbiota under pathological condition and their modulation by berberine is worth further scrutiny (see the following sections).
lP
3.1. Anti-obesity and antihyperlipidemic effects through regulation of the gut microbiota
Jo
ur
na
The antiobesity potential of berberine has been demonstrated in numerous experimental models. Through the AMP-Activated Protein Kinase (AMPK)-dependent and independent mechanisms, berberine can inhibit adipogenesis in experimental animals [50]. In obese mice, berberine administered through peripheral or central route can lower liver weight, hepatic and plasma triglycerides (TGs), and cholesterol contents by promoting AMPK activity and fatty acid oxidation and modulation of expression of genes involved in lipid metabolism. Some of the effects of berberine in obesity could be linked to its ability to modulation of microRNA (miRNA) as shown from its inhibitory effect on 3T3-L1 adipocytes cell differentiation and reduction of TGs contents via increased mRNA expression levels of miRNA-27a and miRNA-27b [51]. This in turn is linked to the negative regulation of the peroxisome proliferator-activated receptors (PPAR)-γ by these miRNA (miRNA-27a). Adipocyte differentiation has also been widely reported as a mechanism for the antiobesity effect of berberine through various distinct mechanisms including suppression of galectin-3 in mouse primary preadipocytes isolated from epididymal white adipose tissues [52]. It also suppresses the cAMPresponse element-binding protein (CREB) phosphorylation and CCAAT-enhancer-binding proteinβ(C/EBPβ) expression at the early stage of 3T3-L1 preadipocyte differentiation [53]. Berberine could also enhance thermogenesis in white adipose tissues [54]. Berberine further regulates lipid metabolism by upregulating hepatic low-density lipoprotein (LDL) receptors through the AMPK-dependent Raf-1 activation pathway [55]. One of the best researched experimental models for the antiobesity effect of berberine is the highfat diet-induced obesity in mice where it has been shown to inhibit adipogenesis [57]. The aniobesity (weight loss), lipid lowering effect of berberine as a function of TGs and cholesterol reduction have been demonstrated in both rats and humans [58]. Through both central and peripheral action that are
distinctly different from the statins, berberine is now known as a potent antiobesity and lipid lowering agent [59,60]. It is based on this plethora of evidences for berberine as weight, lipid and cholesterol lowering agent [26, 61-74] that its mechanism through modulation of the gut microbiota (Table 1) is scrutinised herein.
Jo
ur
na
lP
re
-p
ro of
Table 1. The antiobesity and antihyperlipidemic pharmacology of berberine via modulation of the gut microbiota Bioassay model Dosage Key finding References db/db mice 136.5 mg/kg, i.g. Increase SCFA content in faeces; modulate the Zhang et for 11 weeks ratio of Firmicutes-to-Bacteroidetes; increase al. [62] the proportions of Butyricimonas, Lactobacillus, Coprococcus, Ruminococcus, and Akkermansia; reduce the proportions of Prevotella and Proteus at the genus level. High-fat diet- Added to Increase the abundance of Akkermansia spp. Zhu et al. induced drinking water [63] atherosclerosis in (0.5 g/L) for 14 ApoE-/- mice weeks. High-fat diet- 50 mg/kg twice Enrich Firmicutes and Verrucomicrobia and Shi et al. induced weekly, i.g. for decrease Proteobacteria at the phylum level [64] atherosclerosis in 12 weeks when compared with the disease model. ApoE-/- mice Colorectal cancer Diet supplement Alter the structure of gut microbiota - inhibits Wang et al. development in with 500 ppm of the increase in Verrucomicrobia (phylum level); [65] Akkermansia and increase high-fat diet- berberine for 12 decrease Lachnospiraceae_incertae_ sedis (genus level); min/+ obese Apc weeks trends of increase in Bacteroidetes abundance; mice elevate some SCFAs-producing bacteria. High-fat diet- 100 mg/kg, p.o. Reverse the dysbiosis and a reduction in Sun et al. obese mice for 8 weeks SCFAs (butyric, acetic, propionic, isobutyric, [66] isovaleric, valeric acids), in the colon of obese mice; decrease the Firmicutes/Bacteroidetes ratio under obesity. High-fat diet 150 mg/kg, p.o. Reduce the richness and diversity of the gut Xu et al. obesity model in 6 weeks microbiota: increasing the abundance of [67] rats Fusobacteria and Proteobacteria, and decreasing the abundance of Firmicutes and Actinobacteria; no effect on the abundance of the Bacteroidetes phylum; At the genus level, those increased by berberine under obesity include Fusobacterium, Anaerostipes, Bacteroides and Phascolarctobacterium, Erysipelotrichaceae_Incertae_Sedis, Peptostreptococcaceae_Incertae_Sedis and Escherichia-Shigella; while those decreased include Roseburia, Allobaculum, Oscillibacter, Faecalibacterium, Prevotella Desulfovibrio, Coprococcus, Collinsella and Blautia. High-fat diet‐ 100 mg/kg, p.o. Increased berberine bioavailability correlate Wang et al. induced obese for 10 days in with increase in NR activity. [68] hamsters; animals; 500 mg
in
Sun et al. [69]
200 mg/kg, p.o. for 8 weeks
Reverse the decreased level of Bifidobacterum and Bacteroidete in obesity.
Cao et al. [70]
150 mg/kg containing a formulation with 24 mg/kg of oryzanol and 10 mg/kg of vitamin B6; p.o for 4 weeks 150 mg/kg, p.o. for 4 months
Enrich beneficial bacteria (e.g. Bacteroides, Blautia) and decrease the abundance of Escherichia at the genus level.
Li et al. [71]
ro of
Increase conjugated bile acids in serum and their excretion in faeces; inhibits BSH activity in gut microbiota.
Increase the Bacteroidetes-to-Firmicutes (B/F) ratio in obese rats; At the genus level those enriched include Bacteriodes (SCFAproducing) as Bacteriodetes and those suppressed (Firmicutes) include Dorea, Roseburia, and Blautia; others increased include Anaerofilum, Bilophila (SCFAproducing), and Desulfovibrio. Modulate the gut microbiota (increased the proportion of Firmicutes and reduce the proportion of Bacteroidetes); inhibits the 7αdehydroxylation conversion of cholic acid to deoxycholic acid (decreased elimination of bile acids in the gut). Similar effect for both drugs reduce diversity of gut microbiota; of the 134 OTUs identified, sixty were decreased by both drugs; increase the abundance of those belonging to putative SCFAs-producing bacteria (Allobaculum, Bacteriodes, Blautia, Butyricoccus and Phascolarctobacterium). Reduce bacterial diversity with selective enrichment of putative short-chain fatty acid (SCFAs)-producing bacteria (Blautia and Allobaculum); increase elevations of faecal SCFAs concentration; bacterial list on the increase are Allobaculum, Bacteroides, Blautia, Butyricicoccus, Lactobacillus,
Sun et al. [72]
na
100 mg/kg, i.g. for 2 weeks
ur
High-fat dietinduced hyperlipidaemia model in hamster
lP
re
High-fat-fed obese rats
once daily humans
-p
Hyperlipidaemic and normal subjects High-fat dietinduced obesity in wild type (WT) and FXR knockout (FXRint-/) mice High-fat dietinduced Steatohepatitis and dysbiosis of the gut microbiota in mice High-fat dietinduced hyperlipidaemia in rats
Jo
High-fat dietinduced obesity in rats
High-fat diet-fed obese rats
100 or 200 mg/kg berberine or metformin, i.g. for 8 weeks
100 mg/kg, p.o. for 8 weeks
Gu et al. [26]
Zhang al. [73]
et
Zhang al. [74]
et
Phascolarctobacterium, Parasutterella, Dorea, Clostridium XVIII and Fusobacterium and Klebsiella; those suppressed include Clostridium XlVa, Flavonifractor, Lachnospiracea_incertae_sedis, Roseburia and Clostridium XI. Abbreviations: BSH, bile salt hydrolase; NR, nitroreductases; OTUs, operational taxonomic units; SCFAs, short chain fatty acids.
Jo
ur
na
lP
re
-p
ro of
The association between obesity and change in the gut microbiota has been shown to be the key to the effect of berberine as antiobesity agent. This in a way is also linked to the differential pharmacokinetics of berberine under normal and disease states in the gut microbiota. Wang et al. [68] have shown that berberine is more bioavailable in obese than lean animals owing to the differential microbiota composition. By using the high-fat diet-induced non-alcoholic steatohepatitis model in mice, Cao et al. [70] investigated the effect of berberine on the caecal content of proportions of Bacteroidetes, Firmicutes, Bifidobacteria and Lactobacillus species. The antiobesity effect of berberine in this model was established through the significant reduction in body weight and serum lipids (TG and TC). As a link between obesity and diabetes (see, Section 3.2), the anti-inflammatory mechanism of berberine in this model was also evident given the reduction in the level of proinflammatory cytokines such as IL-1, IL-6 and TNF-α which are known to be the major link between obesity and diabetes. Beyond amelioration of obesity and associated disease markers, berberine could reverse the diseaseassociated suppression of the Lactobacillus and Bifidobacterium levels. The obesity-mediated alteration of the microbial ecology [75] is thus a target for berberine. A similar experiment on the high-fat diet-induced hyperlipidaemia model was conducted in hamsters where berberine treatment effectively showed antihypercholesteraemic effect [26]. This is despite the poor pharmacokinetic profile of berberine through the oral route of administration discussed in Section 2. More importantly, treatment with berberine through an oral route could modulate the proportion of Firmicutes and Bacteroidetes in hypercholesteraemic hamsters. As a note of the Firmicutes-to-Bacteroideteratio (F/B) ratio, it was 1.43 in health animals while it was 0.95 in hypercholesteraemic hamsters before berberine treatment increased it to 1.6 [26]. In the hypocholestrolaemic activity study in rats, Li et al. [71] also demonstrated the ameliorative effects of changes in the serum, urine, liver and faecal metabolites. They noted a higher abundance of Bacteroides, Parabacteroides and Blautia after berberine treatment with a concomitant decrease in the genus Escherichia. The taxon-based analysis by Sun et al. [69,72] further showed that Firmicutes, Bacteroidetes, and Proteobacteria were the major phyla of faecal microbiota in rats while after high-fat-induced obesity, berberine could induce a decline in Firmicutes abundance and a moderately increase in Bacteroidetes ratios. Hence, a higher Bacteroidetes-to-Firmicutes (B/F) ratio was observed in obese animals treated by berberine. They also noted the enriching effects of berberine on Bacteroidaceae and Rikenellaceae families; both belonging to the Bacteroidetes phylum. In contrast, the elevated abundances of Christensenellaceae, Dehalobacteriaceae, Erysipelotrichaceae and Peptococcaceae (all belonging to the Firmicutes phylum) in in obese animals declined after treatment with berberine. This was in addition to the increased Alcaligenaceae (Proteobacteria Phylum) in obese animals after treatment with berberine. The effect of berberine as a lipid-lowering agent has been shown to be linked to the gut via modulation of the turnover of bile acids and subsequently the ileal Farnesoid X receptor (FXR) signalling pathway [69]. As receptors for bile acids and regulator of bile acid and their transporters synthesis, the FXR has close working relationship with the gut microbiota. For example, the gut microbiota is the source of the enzyme bile salt hydrolase (BSH) that hydrolyse bile acids conjugates [76]. Hence, the effect of berberine on FXR signalling is similar with the known effect of antibiotics and probiotics in lipid metabolism via microbial remodelling [77,78].
The study by Sun et al. [66] tried to determine the relationship between the bacteria-derived SCFAs with obesity-related markers. They have shown that the level of six types of SCFAs (butyric acid, acetic acid, propionic acid, isobutyric acid, isovaleric acid, and valeric acid) were reduced in obese mice with the most pronounced effect observed in butyric acid. The partial blockage of obesity and diabetes (see, Section 3.2) was associated with modulation of the gut microbiota (Table 1). Once again, Firmicutes and Bacteroidetes are the most abundant bacteria in the gut microflora at the phylum level but the general trend was for Firmicutes to increase and Bacteroidetes to decrease under obesity. Under this condition, the ratio of F/B in obese animals could be increased by up to 10-folds in obese mice which was suppressed by berberine treatment. At the genus level, berberine could also reverse the relative abundance of Clostridiales.g and Oscillospira under obesity condition [66].
Jo
ur
na
lP
re
-p
ro of
In obese animals, berberine has been shown to suppress weight gain along with critical effect on the gut microbiota. Zhang et al. [73], for example have shown treatment of high-fat diet-induced obese animals both by berberine and metformin led to an increase in the total relative abundance in 7 operational taxonomic units (OTUs) to 10–20% from less than 2%. Of the 7 OTUs, six were shown to be major SCFA-producing bacteria such as Blautia, Bacteriodes, Butyricoccus and Phascolarctobacterium. Unlike other studies, however, they reported that neither an increase of the F/B ratio after drug treatments nor any correlation between F/B ratio and body weight or adiposity index. The most recent experiment by Zhang et al. [62] using the db/db mouse model of obesity, diabetes, and dyslipidaemia showed similar effects (Table 1) where the microbiota modulation by berberine was shown to be involved in its antiobesity effect. The study by Zhang et al. [74] on the effect of berberine on obesity through the gut microbiota was among the most comprehensive since they included 3764 OTUs, contributing to 53.51% of all reads for the he most abundant phyla Firmicutes and 1753 OTUs, contributing to 34.83% of all reads for Bacteroidetes. Other phyla included the Proteobacteria (341 OTUs, contributing to 6.22% of all reads), and Actinobacteria (139 OTUs, contributing to 1.15% of all reads). While higher abundances of the phyla Actinobacteria and Verrucomicrobia were observed in the high-fat diet-obese group than normal animals, and trend was shown to be completely reversed by berberine. They also reported that berberine treatment could increase the faecal concentration of total SCFAs, particularly acetic acid and propionic acid, in obese rats. The trend of change for butyric acid was not significant suggesting some discrepancies among the different studies on the role of individual SCFA in obesity-related pathology. In the study of high-fat diet-induced atherosclerosis development in mice, Shi et al. [64] assessed the effect of berberine in the gut microbiota composition, which was dominated by the Firmicutes and Bacteroidetes, followed by Proteobacteria and Verrucomicrobia at the phyla level. The Firmicutes and Verrucomicrobia appeared to be enriched by berberine treatment while the level of Proteobacteria were suppressed when compared with the disease-model groups. The reduction of atherosclerosis score and inflammation by berberine in high-fat diet-induced atherosclerosis in ApoE-/- mice was similarly coupled with microbiota modulation by berberine: increase the abundance of Akkermansia spp. [63]. Hence, there seem to be an overwhelming evidence to suggest that the effect of berberine in obesity, hyperlipidaemia and cholesterol-induced pathologies could be in part linked to modulation of the gut microbiota. More evidences in other pathologies are discussed in the following sections.
3.2. Antidiabetic effects through gut microbiota regulation The efficacy of berberine in type-2 diabetes (T2D) patients have been effectively demonstrated in recent years [79-81]. Its direct effect on increasing the expression level of insulin receptors and to lower blood glucose level in T2D patients have been shown [82]. Hence, berberine is now known to act as antidiabetic agent through modulation of insulin signalling [83]. It is also often regarded as an insulin sensitizing and insulinotropic agent [84]. Meta-analysis of randomised clinical trial data further suggests the antidiabetic potential of berberine for diabetes [85]. In addition to the effect of berberine
in obesity and hyperlipidaemia states discussed in the previous section, it also acts through several other mechanisms including glucagon-like peptide-1 (GLP-1) release [13,86]. Through activation of the AMPK, berberine can also ameliorate the T2D-associated cardiac dysfunction both in cellular and animal models [87]. In high-fat diet-induced obese mice model and macrophages and 3T3-L1 adipocytes in vitro, berberine could ameliorate inflammation, improve glucose tolerance, reduce the increased expressions of inflammatory mediators (TNF-α, IL-6 and MCP-1) and ameliorate the phosphorylation of JNK and IKKβ, the expression of NF-κB p65 IRS-1 (Ser307). Furthermore, berberine inhibits the phosphorylation of IRS-1 (Ser307) while increasing the phosphorylation of AKT (Ser473) in adipose tissue and cultured adipocytes [88]. In addition, berberine can lower glucose level by inducing glycolysis [89] as well as inhibition of gluconeogenesis [90].
ro of
The antidiabetic effect of berberine through its modulatory effect on the gut microbiota is summarised in Table 2 [56,61,62,67,70,74,91-97]. Some of these effects are similar with what is already known for the well-known antidiabetic agent, metformin, which has a profound effect on the microbial diversity (decrease) in high-fat diet-fed mice even more than in lean mice [98]. Table 2. Antidiabetic effect of berberine associated with alteration of microbiota.
In vivo - 200 mg/kg, p.o. for 10 weeks; in vitro - 10, 50 or 100 µM
na In vivo at 100 mg/kg for 5 days; or in vitro on isolated mouse cecal bacteria at 0.1, 1, and 10 mg/mL for 4 hours in an anaerobic chamber
Jo
ur
In vivo in mice or direct effect on bacteria in vitro
db/db mice
136.5 mg/kg metformin 113.75 mg/kg for 11 weeks
or at i.g
References Pan et al. [91]
-p
High-fat diet-fed mice; hepatocytes and 3T3-L1 adipocytes
Key finding Increase the composition of gut microbiota - the enriched OTUs mainly belong to Firmicutes; ameliorate the changes in dominance of Proteobacteria, Planctomycetes, Bacteroidetes, and Firmicutes; alter the decrease in the ratio of Firmicutes to Bacteroidetes; 32 berberine-OTUs negatively correlate with glucose level. Decrease the relative abundance of BCAA-producing bacteria (order Clostridiales; family Streptococcaceae and genera Streptococcus; Clostridiaceae, and Prevotellaceae (genera Prevotella); increased in abundance include Akkermansia (genus of the phylum Verrucomicrobia). In vivo - Alter intestinal bacteria by reducing Firmicutes and Clostridium cluster XIVa and BSH activity; In vitro alter bacterial physiology and bacterial community composition and function (reduce BSH-expressing bacteria like Clostridium spp); no effect on Bacteroidetes but reduce the Firmicutes/Bacteroidetes ratio. Increase SCFA content in faeces; modulate the ratio of Firmicutes-toBacteroidetes; increase the proportions of Butyricimonas, Lactobacillus, Coprococcus, Ruminococcus, and Akkermansia; reduce the proportions of Prevotella and Proteus.
re
Dosage Diet supplementation at a dose of 30 mg/Kg
lP
Bioassay model Grass carp (Ctenopharyngodon idellus)
Yue [92]
et
al.
Tian et al. [93]
Zhang et al. [62]
200 mg/kg, p.o. for 8 weeks
High-fat obese mice
100 mg/kg, p.o. for 8 weeks; cellular model of CI-H716 cells treated with palmitic acid – berberine at 100 µM 150 mg/kg, p.o. 6 weeks
300 mg berberine three times daily, 0.5 h after each major meal for 8 weeks
200 mg/kg, p.o. for 8 weeks
ur
Patients aged 18-65 years with newly diagnosed T2D with (BMI) > 25 kg/m2 before and 8 weeks after treatment High-fat diet-dietinduced Steatohepatitis and dysbiosis of the gut microbiota in mice High-fat-fed obese rats STZ combined with high-fat diet in Rats High-fat diet-fed obese rats
Reduce the richness and diversity of the gut microbiota; increase the abundance of Fusobacteria and Proteobacteria, and decrease the abundance of Firmicutes and Actinobacteria; no effect on the abundance of the Bacteroidetes phylum. Increase in total Bifidobacterium level, Bifidobacterium longum, Bifidobacterium breve, Bifidobacterium adolescentis, and Bifidobacterium infantis in good correlation (except Bifidobacterium breve) with TNF-α and LPS levels.
Xu et al. [67]
Restore the relative level Bifidobacterium and Bacteroidate.
Cao [70]
150 mg/kg, p.o. for 4 months 100 mg/kg, p.o. for 2 weeks
of
Increase the Bacteroidetes-to-Firmicutes ratio in obese rats; see details in Table 1. Decrease in plasma LPS level by increasing tight junction protein (ZO1) expression. 100 mg/kg, p.o. for Reduce bacterial diversity while 8 weeks selectively enriching putative SCFAproducing bacteria (Blautia and Allobaculum); increase elevations of faecal SCFA concentration; see details in Table 1. Abbreviations: LPS, lipopolysaccharide; TNF-α tumour necrosis factor-α.
Jo
Liu et al. [95]
Sun [66]
et
al.
Chen et al. [96]
lP
High-fat diet obesity model in rats
na
diet-
Cui et al. [94]
ro of
High-fat diet obesity-induced diabetes in rats
Increase the populations of Bacteroidetes, Clostridia, Lactobacillales, Prevotellaceae, and Alloprevotella; reduce those of Bacteroidales, Lachnospiraceae, Rikenellaceae, and Desulfovibrio. Reverse the obesity-induced change in the gut microbiota composition – ameliorate the reduction in protective bacteria like Bifidobacterium and the increased gram negative bacteria like Escherichia coli; ameliorate the increased LPS release into plasma. Modulate the changes in dysbiosis and the diabetes-associated reduction in SCFAs in the colon of obese mice (see Table 1)
-p
500 mg/kg, i.g. for 4 weeks
re
STZ-induced diabetic rats under high-fat, highsucrose diet
et
al.
Sun et al. [72] Shan et al. [97] Zhang et al. [74]
Jo
ur
na
lP
re
-p
ro of
In addition to the antiobesity and lipid lowering effect of berberine in the high-fat diet-induced non-alcoholic steatohepatitis model in mice (see, Section 3.1), Cao et al. [70] have shown a reduction in fasting blood glucose (FBG), insulin, and homeostasis model assessment of insulin resistance (HOMAIR) through alteration of the gut microbiota (Table 2). The link between diabetes and obesity being proinflammatyory cytokines and/or inflammation, the alteration of the structure and abundance of the microbiota in the gut was also associated with the observed anti-inflammatory effect. Moreover, berberine ameliorated the morphological and biochemical (ALT and AST) disease markers while the disease-associated suppression of Lactobacillus and Bifidobacterium levels were reversed. The effect of berberine in reversing the suppressed level of SCFAs in obese mice and increasing the ratio of F/B was coupled with its antidiabetic effect (Sun et al. [66]). In this connection, the more pronounced effect of berberine on butyric acid level was consistent with the effect of butyric acid on improvement of insulin sensitivity and increased energy expenditure in mice [99]. As with the antiobesity effect, the antidiabetic effect of probiotics has been shown to be mediated through butyrateinduced mechanism such as increased GLP-1 release [100]. The effect of berberine on diabetes, obesity, inflammation and microbiota modulation was also similar with metformin when assessed in the db/db mouse model of diabetes [62]. Chen et al. [96] studied the effect of berberine in newly diagnosed T2D and overweight patients. Although, the microbiota population studied was limited to the genus Bifidobacterium, four species (B. longum, B. breve, B. infantis and B. adolescentis) appeared to be enriched after berberine treatment. Moreover, the observed change in these group of bacteria, except for B. breve, were positively correlated with the reduction in the TNF-α and LPS levels induced by berberine. Hence, both the antidiabetic and antiobesity potentials of berberine are somehow linked to its anti-inflammatory effect which were all intern linked to changes in the microbiota population of the Bifidobacterium species. Cui et al. [94] recorded that several biochemical and morphological markers of diabetes could be suppressed by berberine (Table 2). These include increased level of antioxidants, insulin and GLP-1 together with reduction in the level of plasma glucose, lipids and insulin resistance. Along with inhibition of gluconeogenesis and enhanced glycolysis that all confer antidiabetic effect, there was an increase in the populations of Bacteroidetes, Clostridia, Lactobacillales, Prevotellaceae, and Alloprevotella while those of Bacteroidales, Lachnospiraceae, Rikenellaceae, and Desulfovibrio were reduced. They also reported the ratios of F/B in the normal, T2D, and berberine groups were 0.54, 1.09, and 0.73, respectively. Hence, the structural changes along with the F/B ratio in the intestines appears to be positively correlated with blood glucose concentrations in diabetic rats. The study by Cui et al. [94] further established that the Clostridiales and Bacteroidales were the dominant orders in the intestines of all treatment groups in rats: while the relative abundances of Clostridiales (35.91%) and Lactobacillales (2.46%) were lower than that of Bacteroidales (47.31%) in the T2D group, with berberine tended to abolish this order. The study by Liu et al. [95] did not find a significant effect on body weight, visceral fat mass or the visceral fat to body weight ratio following treatment of high-fat-fed obese rats with berberine. They have shown however that the inflammatory components of diabetes were ameliorated along with improvement in insulin resistance as well as insulin receptor and insulin receptor substrate-1 expression in the liver. These effects along with pathological markers such as hepatic steatosis was shown to be ameliorated by berberine together with reversal of the obesity-induced alteration of the gut microbiota composition. In particular, the reduction in protective bacteria like Bifidobacterium and increased gram-negative bacteria like E. coli in obesity and berberine’s ability to reverse this trend was suggested as potential mechanism for its antidiabetic properties. A randomized, double-blind and Placebo-controlled Study under the title “Effectiveness and Safety of Berberine Hydrochloride and Bifidobacterium in People with Abnormal Glucose Level” were conducted in China with 300 participants of newly diagnosed patients with pre-diabetes or T2D. Given Bifidobacterium, as a known probiotic that can modulate the gut microbiota and improve glucose and
-p
ro of
lipid metabolism in animal experiments, the 16-weeks study was designed to investigate the link between the antihyperglycaemic effect of berberine tablets by its own and in combination with bifidobacterium mimetic capsules. The primary outcome is the absolute value of fasting plasma glucose and the results are still awaiting. In fish, the study by Pan et al. [91] revealed that the effect of berberine in glucose level of the serum was associated with structural modulation of the gut microbiota. The enriched OTUs mainly belonging to Firmicutes altered to the dominance of Proteobacteria, Planctomycetes, Bacteroidetes, and Firmicutes during and after berberine feeding; decrease the ratio of F/B; 32 berberine-OTUs were significantly negative correlated with glucose level. Readers should bear in mind that this change was on healthy animals and the trend could be different in diabetic animals. The study by Shan et al. [97] did not directly aimed at the microbiota level but they have shown that fasting insulin, insulin resistance index, plasma LPS level, and ZO1 expression were significantly correlated with increased GLP-2 level. The association between bacterial endotoxemia from the gut origin and T2D/obesity has been routinely established by other studies. All the above-mentioned data for berberine is in line with the well-established role played by the gut microbiota in diabetes pathology. Any condition including sleep deprivation that alter the structure of the gut microbiota is thus associated with the development of inflammation in adipose tissues and insulin resistance in animal studies [101]. Accordingly, both obesity and glucose tolerance could be modulated by targeting the gut microbiota [102]. The high blood glucose level associated with obesity in elderly people was also shown to be linked to changes in the gut microbiota [103]. The differential structure and composition of the gut microbiota in normal and T2D diabetes patients observed in many studies [104-106] also appear to be the therapeutic target for berberine.
re
3.3. Gut inflammation and microbiota
Jo
ur
na
lP
Berberine is among the most potent natural products which ameliorate inflammatory bowel disease and associated disorders [36]. Some the key findings on the role of the gut microbiota modulation for its anti-inflammatory properties in the gut is summarised in Table 3 [62,107-109]. Berberine also ameliorate mucosal barrier alteration and dysfunction under diabetic and other pathological conditions. Gong et al. [110] have shown that diabetic rats are subjected to proinflammatory intestinal changes, altered gut-derived hormones, and 2.77-fold increase in intestinal permeability which were all reversed by berberine treatment. This effect was also associated with the known effect of berberine as anti-inflammatory agent via the TLR4/MyD88/NF-κB signalling pathways in intestinal tissue [110]. By activating the AMPK activity thereby suppressing IFN-γ- and Il-17A-producing lamina propria CD4+ T cells both in vitro and in vivo, berberine can suppress chronic inflammation including under IBD condition [111]. Berberine can modulate the transcription factor nuclear factor erythroid 2-related factor 2 (Nrf2) signalling both in Caco-2 cells and rat model of colitis [112] as shown for many other antiinflammatory natural products [113]. Intestinal barrier function in nonalcoholic fat liver disease (NAFLD) in rats maintained under high-fat diet could also be reversed by berberine along with improvement on anti-inflammatory (LPS and cytokines) and lipid (cholesterol) dysregulation markers [114]. Table 3. Inhibition of gut inflammation by berberine via modulation of the gut microbiota. Bioassay model Diarrhoea from irritable bowel syndrome patients transplanted to rats
Dosage 200 mg/kg, p.o. weeks
for 2
Key finding Alter the level of Faecalibacterium, faecal formate, acetate, and propionate by modulating the gut microbiome composition; decrease
References Jia et al. [107]
DSS-induced colitis in mice
40 mg/kg BBR for 10 days
Zhang et al. [62]
ro of
136.5 mg/kg or metformin at 113.75 mg/kg i.g for 11 weeks
Cui et al. [108]
na
Sequencing on 253 faecal samples from consecutive ITP patients and healthy controls.
lP
re
-p
db/db mice
Firmicutes-to-Bacteroidetes ratio at the phylum level; decrease at the genus level Bacteroides, Faecalibacterium, Ruminococcus, Gemmiger, Roseburia, Clostridium XI, and Lachnospiraceae_incertae_sedis. Reduce serum LPS levels; increase SCFA content in faeces; modulate the ratio of Firmicutes-to-Bacteroidetes; increase the proportions of Butyricimonas, Lactobacillus, Coprococcus, Ruminococcus, and Akkermansia; reduce the proportions of Prevotella and Proteus. Increase the relative abundance of Eubacterium while reducing Desulfovibrio in the disease model; Bacteroides abundance even higher than the level in healthy animals; effect on Treg/Th17 balance was ameliorated after the depletion (by combination of ciprofloxacin and metronidazole treatment) of gut microbiota. Improve the microbial dysbiosis of corticosteroid-resistant ITP patients; reverse the effect of L. bacterium colonization on gut microbiota structure.
Wang et al. [109]
ur
Abbreviations: ITP, Thrombocytopenia; Treg, regulatory T cells.
Jo
The anti-inflammatory effect and amelioration of ulcerative colitis in rats by berberine was shown to be associated with modulation of the gut microbiota [108]. In this DSS-induced colitis model in mice, berberine treatment could recover body weight loss and decreased loss of colon length, mucosal necrosis and the associated inflammation. They also noted the ratio of CD4+IL17A+(Th17) cells in spleen lymphocytes were increased while the proportion of CD4+CD25+Foxp3+(Treg or regulatory T cells) cells in spleen lymphocytes were decreased by berberine treated animals with colitis. Hence, berberine treatment could improve the Treg/Th17 balance in the DSS-induced colitis model. Even though the most abundant phyla in all animal groups were Bacteroidetes, Firmicutes, and Proteobacteria, those treated with berberine have Proteobacteria, Streptococcaceae, Enterococcaceae, and Erysipelotrichale as predominant intestinal flora. While the relative abundance of various groups could be modified by berberine (Table 3), the effect of berberine on the Treg/Th17 balance was lost after the depletion (by combination of ciprofloxacin and metronidazole treatment) of the gut microbiota. Hence, the antiinflammatory effect of berberine in this colitis model was induced through modulation of the
na
lP
re
-p
ro of
microbiota. Based on meta-analysis of twenty-three randomized controlled trials with a total of 1763 patients of active ulcerative colitis, probiotics have been shown to have additional benefit in inducing remission [115]. This is consistent with experimental data in animal studies where probiotics ameliorate colitis by increasing Treg [116]. In this direction, the role of SCFAs, as microbial product to regulate the size and function of the colonic Treg pool and protect against colitis in mice have been established [117]. When the faecal microbiota from diarrhoea-predominant irritable bowel syndrome patients were transplanted to rats, it was shown to induce significant Kupffer cell hyperplasia, hepatic sinusoid hypertrophy, and elevated levels of hepatic TNF-α and interferon-γ and a decrease in the synthesis of ALB [107]. Under this condition, berberine could partially reverse the Kupffer cell hyperplasia, Faecalibacterium, faecal formate, acetate, and propionate levels by modulating the gut microbiome composition. It was also shown that treatment with berberine can significantly change the structure and profile of the faecal microbiome of the disease group (Table 3). As discussed for obesity and diabetes conditions, Rajilić-Stojanović et al. [118] have shown that the microbiota of IBS patients when compared with controls, had a “2-fold increased ratio of the Firmicutes to Bacteroidetes resulting from an approximately 1.5-fold increase in numbers of Dorea, Ruminococcus, and Clostridium spp; a 2-fold decrease in the number of Bacteroidetes; a 1.5-fold decrease in numbers of Bifidobacterium and Faecalibacterium spp; and, when present, a 4-fold lower average number of methanogens”. While the degree of changes may depend on the severity of the diseases and doses of therapeutic agents, the effect of berberine appears to be in line with these observations. Wang et al. [109] have shown that dysbiosis was detected in the gut microbiome of Thrombocytopenia (ITP) patients with Lachnospiraceae bacterium, Clostridium asparagiforme were overrepresented while Bacteroides spp was depleted when compared with healthy controls. In this case, berberine treatment could improve the microbial dysbiosis of corticosteroid-resistant ITP patients (Table 3). Interestingly, berberine but not antibiotics, enhance the response to corticosteroid therapy by reversing the effect of L. bacterium colonization on gut microbiota structure. This of course needs further research to establish how modulation of L. bacterium could lead to the observed effect. In the antidiabetic activity studies using db/db mice, Zhang et al. [62] showed that berberine and metformin could reverse the disease-mediated reduction in the level of occludin and ZO1 tight junction proteins along with increased SCFA content in faeces and/or reversal of the altered microbiota composition (Table 3). 3.4. Other organoprotective effects
Jo
ur
Given the diverse pharmacological effects of berberine through multiple mechanisms including general anti-inflammatory and antioxidants properties, its organoprotective effect is not surprising. By regulating autophagic flux, berberine can induce hepatoprotective effect under high level of cholesterol [66]. Hence, it induces neuroprotective effects in cellular models such as SH-SY5Y and PC12 cells [119,120], in animal models [121,122] and under clinical conditions [123]. The hepatoprotective [124,125], cardioprotective including in humans [126-128] and nephroprotective [129,130] effects, among others, of berberine have been well-established. On these bases and the organoprtective effects under obesity, hyperepidemic and diabetes discussed in the preceding sections, it is interesting to see the link between its organoprotective and modulatory effects in the gut microbiota. Guan et al. [131] have studied the role played by the colon microbiota in the ameliorative effect of berberine on the bleomycin-induced pulmonary fibrosis (PF) in mice. While the mechanisms involved activation of PPAR-γ in lung tissues, they have shown that it was a result of hepatocyte growth factor (HGF) expression in colonic fibroblasts. In this connection, the LPS-induced hepatocyte proliferation via stimulation of HGF has been shown to be suggested as the link between the gut microbiota and liver regeneration [132]. In the gut of liver cirrhosis patients, potentially pathogenic bacteria including the Enterobacteriaceae and Streptococcaceae have been shown to be predominant while the beneficial
bacteria such as Lachnospiraceae exit at lower level [133]. Agents like berberine with a profound effect on the structure of the gut microbiota in health and diseases are thus likely to modulate diseases through such mechanisms. Evidence for the direct link was further provided by the study of Quin et al. [134] which showed that berberine could ameliorate the diethylnitrosamine-induced hepatotoxicity and intestinal damage induced by penicillin or DSS. They have also used faecal microbiota transplantation experiment to demonstrate that the observed beneficial effect of berberine was mediated by homeostatic alteration in the gut microbiota. These data are also consistent with those by Jia et al. [135] which revealed that berberine can alleviate some of the inflammatory damage in germfree rats subjected to faecal microbiota from IBS patients. Other effect of berberine linked to the gut microbiota is related to periodontal bone loss [136]. 3.5. Cancer
Jo
ur
na
lP
re
-p
ro of
Noting the high inter-individual variability in the mice gut microbial composition, Wang et al. [137] studied colorectal cancer development in high-fat obese Apc min/+ mice. As with other experiments discussed in the previous sections, the predominant gut microbiota of wild type mice taxa at the phylum level were Firmicutes (55.7%) and Bacteroidetes (42.28%); and on the lower scale, Proteobacteria (1.69%) and Verrucomicrobia (0.11%). The individual variation in these groups could be up to 55% (Bacteroidetes and Firmicutes) in the wild type mice, while the level of Verrucomicrobia increases (wild type and Apc min/+ mice) by high-fat diet, treatment with berberine appear to ameliorate both the structural changes in microbiota and colorectal cancer development. The association between the effect of berberine on colorectal cancer and microbiota regulation was also investigated by Gao et al. [138]. Their study characterized the faecal microbiota, also known as fungal signature, in 131 subjects, comprising polyp and colorectal cancer (CRC) patients. They reported a distinct fungal dysbiosis and an alteration in the fungal network in polyp and CRC pathogenesis. Whether this pattern could be reversed by natural products such as berberine remains to be investigated. The study by Yu et al. [139] employed a potent carcinogen, 1,2-dimethylhydrazine (DMH) or Fusobacterium nucleatum in mice in the presence or absence of berberine. Treatment with F. nucleatum, for example, could increase the level of opportunistic pathogens such as Tenericutes and Verrucomicrobia both in in wild-type and in mice treated with DMH. Berberine was able to ameliorate this bacterial compositional change along with modulation of inflammatory markers: IL-21/22/31, CD40L and the expression of p-STAT3, p-STAT5 and p-ERK1/2, when compared with mice fed with F. nucleatum alone. The levels of opportunistic pathogens, such as Fusobacterium, Streptococcus and Enterococcus spp. gradually increased during the colorectal adenoma-carcinoma sequence in human faecal and mucosal samples. Readers should note that berberine is by far one of the best studied natural products for direct toxicity to cancer cells such as breast cancer [140], colorectal [141], lung [142], hepatocarcinoma [143], leukaemia [144], etc. By interfering signalling pathways such as the AMPK [145], PI3K/AKT [146,147], miRNA [148,149], and prostaglandin [150], berberine has been shown to suppress cancer metastasis. As an adjuvant or combination therapy, berberine has also been shown to enhance the activity of anticancer drugs such as tamoxifen [151], vincristine [152], cisplatin [153], etc. On these bases and the observed effect of berberine on the gut microbiota, berberine is an example of a natural products that acts through polypharmacology principles. General Summary and Conclusion Berberine is a multifunctional natural product with diverse therapeutic applications. As a potent inhibitor of enzymes such as acetylcholinesterase and its ability to alter the amyloid β-induced pathological changes, its therapeutic potential in neurodegenerative diseases such as Alzheimer’s disease has been advocated [4]. Berberine also possesses antioxidant and anti-inflammatory effects in vivo and its plethora of pharmacological effects as organoprotective agent could be linked to such
lP
re
-p
ro of
properties. The therapeutic potential of berberine is thus through acting on multiple targets of the polypharmacology principle that has been shown for many natural products [22]. Evidences presented in this paper now appear to also show that the effect of berberine is linked to the diverse effects of the gut microbiota in health and disease as depicted in Figure 2.
Jo
ur
na
Figure 2. Modulation of the gut microbiota by berberine in health and disease. The polypharmacology of berberine is associated with the diverse effect of the gut microbiota in health and disease. Berberine has a poor bioavailability and its metabolism and pharmacokinetics are related to the activity of the microbiota. Under normal conditions, the structure and composition of the gut microbiota, partly through increased production of SCFAs, promote health. The reduced level of infection and LPS means low level of inflammation both in the gut and in the circulation which has also implication to improved lipid metabolism and insulin sensitivity. Under pathological conditions, the gut microbiota composition is in favour of pathogenic bacteria proliferation and the resulting gut inflammation with compromised intestinal barrier allow high level of systemic LPS. Altered lipid metabolism and insulin sensitivity are associated with such changes leading to the development of diseases such as hyperlipidaemia-associated cardiovascular diseases, diabetes, neurodegenerative diseases and organ disfunction associated with inflammation and oxidative stress (e.g., liver, kidney, and pulmonary dysfunctions). While berberine has multiple effects through enzyme/receptor and cell signalling mechanisms, a growing evidence now also suggest that it acts through modulation of the gut microbiota structure and composition.
The evidences on the modulation of microbiota by berberine showed a great deal of variability to the extent of changes both in quantitative and qualitative manor. While some evidences show, alteration in F/B ratio, some studies show no effect on this ratio. Although the general trend is that
berberine reverses the suppressed level of SCFAs under pathological conditions, there is also data variability related to which individual SCFA is more affected by berberine. Most of these data variations are also attributed to the inter-individual variations in the composition of the gut microbiota. The effect of berberine on the gut microbiota appears to be similar with the general pharmacology associated with the therapeutic application of probiotics, dietary fibres and other drugs such as metformin. With the call for more scientific research on the above-mentioned data variations, the polypharmacology of berberine is in part explained by its role in modulation of the gut microbiota. Conflicts of Interest: The authors declare no conflict of interest.
Funding: This work did not receive any financial support from either internal or external sources.
References
6. 7. 8.
9.
10.
11.
ro of
Jo
12.
-p
5.
re
4.
lP
3.
na
2.
D. Potdar, R.R. Hirwani, S. Dhulap, Phyto-chemical and pharmacological applications of Berberis aristate, Fitoterapia, 83 (5) (2012) 817-830. A. Singh, S. Duggal, N. Kaur, J. Singh, Berberine: Alkaloid with wide spectrum of pharmacological activities, J Nat Prod 3 (2010) 64-75. S. Habtemariam, The hidden treasure in Europe’s garden plants: Case examples; Berberis darwinni and Bergenia cordifolia, Medicinal & Aromatic Plants 2013, 2, 4. S. Habtemariam, The therapeutic potential of Berberis darwinii stem-bark: quantification of berberine and in vitro evidence for Alzheimer’s disease therapy, Nat. Prod. Commun. 6 (8) (2011) 1089–1090. A. Singh, V. Bajpai, M. Srivastava, K.R. Arya, B. Kumar, Rapid screening and distribution of bioactive compounds in different parts of Berberis petiolaris using direct analysis in real time mass spectrometry, J Pharm Anal 5 (5) (2015) 332-335. R. Suau, R. Rico, J.M. López-Romero, F. Nájera, A. Cuevas, Isoquinoline alkaloids from Berberis Vulgaris subsp. Australis Phytochemistry 49 (8) (1998) 2545-2549. ACS. Berberine. https://www.acs.org/content/acs/en/molecule-of-theweek/archive/b/berberine.html (Accessed, 6 January 2020) D.G. Kim, J.W. Choi, I.J. Jo, M.J. Kim, H.S. Lee, S.H. Hong, et al., Berberine ameliorates lipopolysaccharide-induced inflammatory responses in mouse inner medullary collecting duct-3 cells by downregulation of NF-κB pathway, Mol Med Rep (2019) doi: 10.3892/mmr.2019.10823. M. Takahara, A. Takaki, S. Hiraoka, T. Adachi, Y. Shimomura, H. Matsushita, et al., Berberine improved experimental chronic colitis by regulating interferon-γ- and IL-17A-producing lamina propria CD4+ T cells through AMPK activation, Sci Rep 9(1) (2019) 11934. C. Gong, X. Hu, Y. Xu, J. Yang, L. Zong, C. Wang, et al., Berberine inhibits proliferation and migration of colorectal cancer cells by downregulation of GRP78, Anticancer Drugs (2019) doi: 10.1097/CAD.0000000000000835. F. Jin, T. Xie, X. Huang, X. Zhao, Berberine inhibits angiogenesis in glioblastoma xenografts by targeting the VEGFR2/ERK pathway, Pharm Biol 56 (1) (2018) 665-671. Y. Wang, S. Zhang, Berberine suppresses growth and metastasis of endometrial cancer cells via miR-101/COX-2, Biomed Pharmacother 103 (2018) 1287-1293. Y. Yu, L. Liu, X. Wang, X. Liu, X. Liu, L. Xie, et al., Modulation of glucagon-like peptide-1 release by berberine: in vivo and in vitro studies, Biochem Pharmacol, 79 (7) (2010) 1000-1006. Y. Zhang, X. Li, D. Zou W. Liu, J. Yang, N. Zhu, et al., Treatment of type 2 diabetes and dyslipidemia with the natural plant alkaloid berberine, J Clin Endocrinol Metab 93 (7) (2008) 25592565. H. Zhang, J. Wei, R. Xue J.D. Wu, W. Zhao, Z.Z. Wang, et al., Berberine lowers blood glucose in type 2 diabetes mellitus patients through increasing insulin receptor expression, Metabolism 59 (2010) 285–292.
ur
1.
13. 14.
15.
Jo
ur
na
lP
re
-p
ro of
16. W.S. Kim, Y.S. Lee, S.H. Cha, H.W. Jeong, S.S. Choe, M.R. Lee, et al., Berberine improves lipid dysregulation in obesity by controlling central and peripheral AMPK activity, Am J Physiol Endocrinol Metab 296 (4) (2009) E812-E819. 17. G. Derosa, P. Maffioli, A.F. Cicero, Berberine on metabolic and cardiovascular risk factors: an analysis from preclinical evidences to clinical trials, Expert Opin Biol Th 12 (2012) 1113–1124. 18. Y. Yu, M. Zhang, Y. Hu, Y. Zhao, F. Teng, X. Lv, et al., Increased bioavailable berberine protects against myocardial ischemia reperfusion injury through attenuation of NFκB and JNK signaling pathways, Int Heart J 59 (6) (2018) 1378-1388. 19. K. Wang, Q. Chen, N. Wu, Y. Li, R. Zhang, J. Wang, et al., Berberine Ameliorates Spatial Learning Memory Impairment and Modulates Cholinergic Anti-Inflammatory Pathway in Diabetic Rats. Front Pharmacol 10 (2019) 1003. 20. S. Ghotbi-Ravandi, M. Shabani, H. Bashiri, M. Saeedi Goraghani, M. Khodamoradi, M. Nozari, Ameliorating effects of berberine on MK-801-induced cognitive and motor impairments in a neonatal rat model of schizophrenia, Neurosci Lett 706 (2019) 151-157. 21. S. Sadraie, Z. Kiasalari, M. Razavian, S. Azimi, L. Sedighnejad, S. Afshin-Majd, et al., Berberine ameliorates lipopolysaccharide-induced learning and memory deficit in the rat: insights into underlying molecular mechanisms, Metab Brain Dis 2019 34 (1) 245-255. 22. S. Habtemariam, Going back to the good old days: The merit of crude plant drug mixtures in the 21st century, Int J Complement Alt Med 6 (2) (2017) 00182 23. W. Chen, Y.Q. Miao, D.J. Fan, S.S. Yang, X. Lin, L.K. Meng, et al., Bioavailability study of berberine and the enhancing effects of TPGS on intestinal absorption in rats, AAPS PharmSciTech 12 (2011) 705–711. 24. G.Y. Pan, G.J. Wang, X.D. Liu, J.P. Fawcett, Y.Y. Xie, The involvement of P‐glycoprotein in berberine absorption, Pharmacol Toxicol 91 (2002) 193–197. 25. Y.T. Liu, H.P. Hao, H.G. Xie, L. Lai, Q. Wang, C.X. Liu, et al., Extensive intestinal first-pass elimination and predominant hepatic distribution of berberine explain its low plasma levels in rats. Drug Metab Dispos 38 (2010) 1779–1784. 26. S.H. Gu, B. Cao, R.B. Sun, Y.Q. Tang, J.L. Paletta, X.L. Wu, et al., A metabolomic and pharmacokinetic study on the mechanism underlying the lipid-lowering effect of orally administered berberine, Molecular Biosystems 11 (2) (2015) 463-474. 27. W. Hua, L. Ding, Y. Chen, B. Gong, J. He, G. Xu, Determination of berberine in human plasma by liquid chromatography–electrospray ionization–mass spectrometry, J Pharmaceut Biomed 44 (2007) 931–937. 28. X.S. Tan, J.Y. Ma, R. Feng, C. Ma, W.J. Chen, Y.P. Sun, et al., Tissue distribution of berberine and its metabolites after oral administration in rats. PloS One 8 (2013) e77969. 29. R. Feng, Z.X. Zhao, S.R. Ma, F. Guo, Y. Wang, J.D. Jiang, Gut Microbiota-regulated pharmacokinetics of berberine and active Metabolites in Beagle dogs after oral administration, Front Pharmacol 9 (2018) 214. 30. H.W. Xin, X.C. Wu, Q. Li, A.R. Yu, M.Y. Zhong, Y.Y. Liu, The effects of berberine on the pharmacokinetics of cyclosporin A in healthy volunteers, Methods Find Exp Clin Pharmacol 28 (1) (2006) 25-29. 31. Y.F. Lyu, Y.F. Zhang, M.B. Yang, L. Lin, X. Yang, S.C.K. Cheung, et al., Pharmacokinetic interactions between metformin and berberine in rats: Role of oral administration sequences and microbiota, Life Sciences 235 (2019) 116818. 32. Y. Guo, Y.C. Zhang, W.H. Huang, F.P. Selwyn, C.D. Klaassen, Dose-response effect of berberine on bile acid profile and gut microbiota in mice, BMC Complement Altern Med 16 (1) (2016) 394. 33. R.N. Alolga, Y. Fan, Z. Chen, L.W. Liu, Y.J. Zhao, J. Li, et al., Significant pharmacokinetic differences of berberine are attributable to variations in gut microbiota between Africans and Chinese, Sci Rep 6 (2016) 27671. 34. R. Feng, J.W. Shou, Z.X. Zhao, C.Y. He, C. Ma, M. Huang, et al., Transforming berberine into its intestine-absorbable form by the gut microbiota, Sci Rep 5 (2015) 12155.
Jo
ur
na
lP
re
-p
ro of
35. Y. Wang, J.W. Shou, X.Y. Li, Z.X. Zhao, J. Fu, C.Y. He, et al., Berberine-induced bioactive metabolites of the gut microbiota improve energy metabolism, Metab Clin Exp 70 (2017) 72-84. 36. S. Habtemariam, Berberine and inflammatory bowel disease: A concise review, Pharmacol Res 113 (Pt A) (2016) 592-599. 37. M.L. Freile, F. Giannini, G. Pucci, A. Sturniolo, L. Rodero, O. Pucci, et al., Antimicrobial activity of aqueous extracts and of berberine isolated from Berberis heterophylla, Fitoterapia 74 (7–8) (2003) 702– 705. 38. K. Karaosmanoglu, N.A. Sayar, I.A. Kurnaz, B.S. Akbulut, Assessment of berberine as a multitarget antimicrobial: a multi-omics study for drug discovery and repositioning, OMICS 18 (1) (2014) 42–53. 39. Z. Lv, G. Peng W. Liu, H. Xu, J. Su, Berberine blocks the relapse of Clostridium difficile infection in C57BL/6 mice after standard vancomycin treatment, Antimicrob Agents Chemother 59 (7) (2015) 3726-3735. 40. C. Chen, C. Tao, Z. Liu, M. Lu, Q. Pan, L. Zheng, et al., Randomized clinical trial of berberine hydrochloride in patients with diarrhea-predominant irritable bowel syndrome, Phytother Res 29 (11) (2015) 1822–1827. 41. M. Cernakova, D. Kostalova, Antimicrobial activity of berberine - a constituent of Mahonia aquifolium, Folia Microbiol (Praha) 47 (4) (2002) 375–378. 42. S.H. Chae, I.H. Jeong, D.H. Choi, J.W. Oh, Y.J. Ahn, Growth-inhibiting effects of Coptis japonica rootderived isoquinoline alkaloids on human intestinal bacteria. J Agric Food Chem 47 (3) (1999) 934– 938. 43. V.T. Do, B.G. Baird, D.R. Kockler, Probiotics for maintaining remission of ulcerative colitis in adults. Ann Pharmacother 44 (3) (2010) 565–571. 44. D. Haller, J.M. Antoine, S. Bengmark, P. Enck, G.T. Rijkers, I. Lenoir-Wijnkoop, Guidance for substantiating the evidence for beneficial effects of probiotics: probiotics in chronic inflammatory bowel disease and the functional disorder irritable bowel syndrome, J Nutr 140 (3) (2010) 690S– 697S. 45. A.J. Riquelme, M.A. Calvo, M.A. Guzmán, M.S. Depix, P. García, C.M. Pérez, et al., Saccharomyces cerevisiae fungemia after Saccharomyces boulardii treatment in immunocompromised patients, J Clin Gastroenterol 36 (1) (2003) 41–43. 46. W. Sandborn, R. McLeod, D. Jewell, Pharmacotherapy for inducing and maintaining remission in pouchitis, Cochrane Database Syst Rev 2 (2002) CD001176. 47. S.J. Yue, J. Liu, W.X. Wang, A.T. Wang, X.Y. Yang, H.S. Guan, et al., Berberine treatment-emergent mild diarrhea associated with gut microbiota dysbiosis, Biomed Pharmacother 116 (2019) 109002. 48. H.Y. Zhang, X.S. Piao, Q. Zhang, P. Li, J.Q. Yi, J.D. Liu, et al., The effects of Forsythia suspensa extract and berberine on growth performance, immunity, antioxidant activities, and intestinal microbiota in broilers under high stocking density, Poultry Science 92 (8) (2013) 1981-1988. 49. R.E. Ley, M. Hamady, C. Lozupone, P.J. Turnbaugh, R.R. Ramey, J.S. Bircher, et al., Evolution of mammals and their gut microbes, Science 320 (5883) (2008) 1647-1651. 50. Y. Yang, F. Liu, R. Lu, J. Jia, Berberine Inhibits Adipogenesis in Porcine Adipocytes via AMPActivated Protein Kinase-Dependent and -Independent Mechanisms, Lipids 54 (11-12) (2019) 667678. 51. Y.Y. Wu, X.M. Huang, J. Liu, Y. Cha, Z.P. Chen, F. Wang, et al., Functional study of the upregulation of miRNA-27a and miRNA-27b in 3T3-L1 cells in response to berberine, Mol Med Rep 14 (3) (2016) 2725-31. 52. C. Wang, Y. Wang, S.R. Ma, Z.Y. Zuo, Y.B. Wu, W.J. Kong, et al., Berberine inhibits adipocyte differentiation, proliferation and adiposity through down-regulating galectin-3, Sci.Rep 9 (1) (2019) 13415. 53. J. Zhang H. Tang R. Deng N. Wang Y. Zhang Y. Wang et al., Berberine suppresses adipocyte differentiation via decreasing CREB transcriptional activity, PLoS One 10 (4) (2015) e0125667.
Jo
ur
na
lP
re
-p
ro of
54. Z. Zhang, H. Zhang, B. Li, X. Meng, J. Wang, Y. Zhang, et al., Berberine activates thermogenesis in white and brown adipose tissue, Nat Commun 5 (2014) 5493. 55. Z. Li, J.D. Jiang, W.J. Kong, Berberine up-regulates hepatic low-density lipoprotein receptor through ras-independent but AMP-activated protein kinase-dependent Raf-1 activation, Biol Pharm Bull 37 (2014) 1766–1775. 56. H.D. Sun, Q. Liu, H. Hu, Y.S. Jiang, W.T. Shao, Q.H. Wang, et al., Berberine ameliorates blockade of autophagic flux in the liver by regulating cholesterol metabolism and inhibiting COX2prostaglandin synthesis, Cell Death Dis 9 (2018) 824 57. Y. Hu, G.E. Davies, Berberine inhibits adipogenesis in high-fat diet-induced obesity mice, Fitoterapia 81 (2010) 358–366. 58. Y. Hu, E.A. Ehli, J. Kittelsrud, P.J. Ronan, K. Munger, T. Downey, et al., Lipid-lowering effect of berberine in human subjects and rats, Phytomedicine 19 (10) (2012) 861-867. 59. W.S. Kim, Y.S. Lee, S.H. Cha, H.W. Jeong, S.S. Choe, M.R. Lee, et al., Berberine improves lipid dysregulation in obesity by controlling central and peripheral AMPK activity, Am J Physiol Endocrinol Metab 296 (4) (2009) E812-9. 60. W. Kong, J. Wei, P. Abidi, M. Lin, S. Inaba, C. Li, et al., Berberine is a novel cholesterol-lowering drug working through a unique mechanism distinct from statins, Nat Med 10 (2004) 1344–1351. 61. H.H. Guo, C. Ma, W.S. Zheng, Y. Luo, C. Li, X.L. Li, et al., Dual-Stimuli-Responsive Gut MicrobiotaTargeting Berberine-CS/PT-NPs Improved Metabolic Status in Obese Hamsters, Adv. Funct. Mater. 29 (14) (2019) doi: 10.1002/adfm.201808197 62. W. Zhang, J.H. Xu, T. Yu, Q.K. Chen, Effects of berberine and metformin on intestinal inflammation and gut microbiome composition in db/db mice, Biomed Pharmacother 118 (2019) 109131. 63. L. Zhu, D.Y. Zhang, H. Zhu, J.M. Zhu, S.G. Weng, L. Dong, et al., Berberine treatment increases Akkermansia in the gut and improves high-fat diet-induced atherosclerosis in Apoe(-/-) mice, Atherosclerosis 268 (2018) 117-126. 64. Y.F. Shi, J.X. Hu, J. Geng, T.T. Hu, B.J. Wang, W.T. Yan, et al., Berberine treatment reduces atherosclerosis by mediating gut microbiota in apoE-/- mice, Biomed Pharmacother 107 (2018) 1556-1563. 65. H. Wang, L.N. Guan, J. Li, M.D. Lai, X.D. Wen, The effects of berberine on the gut microbiota in Apc (min/+) mice fed with a high fat diet, Molecules 23 (9) (2018) pii: E2298. 66. Y. Sun, C. Jin, X. Zhang, W. Jia, J. Le, J. Ye, Restoration of GLP-1 secretion by Berberine is associated with protection of colon enterocytes from mitochondrial overheating in diet-induced obese mice, Nutr Diabetes 8 (1) (2018) 53. 67. J.H. Xu, X.Z. Liu, W. Pan, D.J. Zou, Berberine protects against diet-induced obesity through regulating metabolic endotoxemia and gut hormone levels, Mol Med Rep 15 (5) (2017) 2765-2787. 68. Y. Wang, Q. Tong, J.W. Shou, Z.X. Zhao, X.Y. Li, X.F. Zhang, et al., Gut microbiota-mediated personalized treatment of hyperlipidemia using berberine, Theranostics 7 (9) (2017) 2443-2451. 69. R.B. Sun, N. Yang, B. Kong, B. Cao, D. Feng, X.Y. Yu, et al., Orally administered berberine modulates hepatic lipid metabolism by altering microbial bile acid metabolism and the intestinal FXR signaling pathway, Mol Pharmacol 9 (2) (2017) 110-122. 70. Y. Cao, Q. Pan, W. Cai, F. Shen, G.Y. Chen, L.M. Xu, et al., Modulation of gut microbiota by berberine improves steatohepatitis in high-fat diet-fed BALB/C mice, Arch Iran Med 19 (3) (2016) 197-203. 71. M. Li, X.B. Shu, H.C. Xu, C.L. Zhang, L.L. Yang, L. Zhang, et al., Integrative analysis of metabolome and gut microbiota in diet-induced hyperlipidemic rats treated with berberine compounds, J Trans Med 14 (1) (2016) 237. 72. H.L. Sun, N.J. Wang, Z. Cang, C.X. Zhu, L. Zhao, X.M. Nie, et al., Modulation of microbiota-gutbain axis by berberine resulting in improved metabolic status in high-fat diet-fed rats, Obesity Facts 9 (6) (2016) 365-378.
Jo
ur
na
lP
re
-p
ro of
73. X. Zhang, Y.F. Zhao, J. Xu, Z.S. Xue, M.H. Zhang, X.Y. Pang, et al., Modulation of gut microbiota by berberine and metformin during the treatment of high-fat diet-induced obesity in rats, Sci Rep 5 (2015) 14405. 74. X. Zhang, Y.F. Zhao, M.H. Zhang, X.Y. Pang, J. Xu, C.Y. Kang, et al., Structural changes of gut microbiota during berberine-mediated prevention of obesity and insulin resistance in high-fat diet-fed rats, Plos One 7 (8) (2012) e42529. 75. R.E. Ley, F. Bäckhed, P. Turnbaugh, C.A. Lozupone, R.D. Knight, J.I. Gordon, Obesity alters gut microbial ecology, Proc Natl Acad Sci USA 102 (2005) 11070–11075. 76. M. Begley, C. Hill C.G. Gahan, Bile salt hydrolase activity in probiotics, Appl Environ Microbiol. 72 (3) (2006) 1729-1738. 77. I. De Smet, L. Van Hoorde, M. Vande Woestyne, H. Christiaens, W. Verstraete, Significance of bile salt hydrolytic activities of lactobacilli, J Appl Bacteriol 79 (3) (1995) 292-301. 78. F. Li, C. Jiang, KW. Krausz, Y. Li, I. Albert, H. Hao, et al., Microbiome remodelling leads to inhibition of intestinal farnesoid X receptor signalling and decreased obesity, Nat Commun 4 (2013) 2384. 79. J. Lan, Y. Zhao, F. Dong, Z. Yan, W. Zheng, J. Fan, et al., Meta-analysis of the effect and safety of berberine in the treatment of type 2 diabetes mellitus, hyperlipemia and hypertension, J Ethnopharmacol 161 (2015) 69-81 80. J. Yin, H. Xing, J. Ye, Efficacy of berberine in patients with type 2 diabetes mellitus, Metabolism 57 (2008) 712–717. 81. Y. Zhang, X. Li, D. Zou, W. Liu, J. Yang, N. Zhu, et al., Treatment of type 2 diabetes and dyslipidemia with the natural plant alkaloid berberine, J Clin Endocrinol Metab 93 (7) (2008) 255965. 82. H. Zhang, J. Wei, R. Xue, J-D. Wu, W. Zhao, Z.Z. Wang, et al., Berberine lowers blood glucose in type 2 diabetes mellitus patients through increasing insulin receptor expression. Metabolism 59 (2010) 285–292. 83. L.Z. Liu, S.C. Cheung, L.L. Lan, S.K. Ho, H.X. Xu, J.C. Chan, et al., Berberine modulates insulin signaling transduction in insulin-resistant cells, Mol Cell Endocrinol 317 (2010) 148–153. 84. B-S. Ko, S.B. Choi, S.K. Park, J.S. Jang, Y.E. Kim, Park, S. Insulin sensitizing and insulinotropic action of berberine from Cortidis rhizome, Biol Pharm Bull 28 (2005) 1431–1437. 85. H. Dong, Y. Zhao, L. Zhao, F. Lu, The effects of berberine on blood lipids: a systemic review and meta-analysis of randomized controlled trials, Planta Med 79 (2013) 437-446. 86. S.S. Lu, Y.L. Yu, H.J. Zhu, X.D. Liu, L. Liu, Y.W. Liu, et al. Berberine promotes glucagon-like peptide-1 (7–36) amide secretion in streptozotocin-induced diabetic rats, J Endocrinol 200 (2009) 159–165. 87. W. Chang, M. Zhang, Z. Meng, Y. Yu, F. Yao, G.M. Hatch, et al., Berberine treatment prevents cardiac dysfunction and remodeling through activation of 5’-adenosine monophosphateactivated protein kinase in type 2 diabetic rats and in palmitate-induced hypertrophic H9c2 cells, Eur J Pharmacol 769 (2015) 55–63. 88. J. Yin, Z. Gao, D. Liu, Z. Liu, J. Ye, Berberine improves glucose metabolism through induction of glycolysis, Am J Physiol Endocrinol Metab 294 (2008) E148–E156. 89. L.F. Ye, S. Liang, C. Guo, X.Z. Yu, J. Zhao, H. Zhang, et al., Inhibition of M1 macrophage activation in adipose tissue by berberine improves insulin resistance, Life Sci 166 (2016) 82-91. 90. X. Xia, J. Yan, Y. Shen, K. Tang, J. Yin, Y. Zhang, et al., Berberine improves glucose metabolism in diabetic rats by inhibition of hepatic gluconeogenesis, PLoS One 6 (2011) e16556. 91. H.J. Pan, Z.F. Li, J. Xie, D. Liu, H.J. Wang, D.G. Yu, et al., Berberine influences blood glucose via modulating the gut microbiome in grass carp, Front Microbiol 10 (2019) 1066.
Jo
ur
na
lP
re
-p
ro of
92. S.J. Yue, J. Liu, A.T. Wang, X.T. Meng, Z.R. Yang, C. Peng, et al., Berberine alleviates insulin resistance by reducing peripheral branched-chain amino acids, Am J Physiol Endocrinol Metab 316 (1) (2019) E73-E85. 93. Y. Tian, J.W. Cai, W. Gui, R.G. Nichols, I. Koo, J.T. Zhang, et al., Berberine directly sffects the gut microbiota to promote intestinal farnesoid X receptor activation, Drug Metab Dispos 47 (2) (2019) 86-93. 94. H.X. Cui, Y.N. Hu, J.W. Li, K. Yuan, Hypoglycemic mechanism of the berberine organic acid salt under the synergistic effect of intestinal flora and oxidative stress, Oxid Med Cell Longev 2018 (2018) 8930374. 95. D. Liu, Y.Y. Zhang, Y.H. Liu, L.Q. Hou, S.Y. Li, H.M. Tian, et al., Berberine modulates gut microbiota and reduces insulin resistance via the TLR4 signaling pathway, Exp Clin Endocrinol Diabets 126 (8) (2018) 513-520. 96. L.L. Chen, W.S. Lu, Y.S. Li, Berberine ameliorates type 2 diabetes via modulation of Bifidobacterium species, tumor necrosis factor-alpha, and lipopolysaccharide, Int. J Clin Exp Med 9 (6) (2016) 9365-9372. 97. C.Y. Shan, J.H. Yang, Y. Kong, X.Y. Wang, M.Y. Zheng, Y.G. Xu, et al., Alteration of the intestinal barrier and GLP2 secretion in Berberine-treated type 2 diabetic rats, J Endocrinol 218 (3) (2013) 255262. 98. H. Lee, G. Ko, Effect of metformin on metabolic improvement and gut microbiota, Appl Environ Microbiol 80 (2014) 5935–5943. 99. Z. Gao, J. Yin, J. Zhang, R.E. Ward, R.J. Martin, M. Lefevre, et al., Butyrate improves insulin sensitivity and increases energy expenditure in mice, Diabetes 5 (2009) 1509–1517. 100. H. Yadav, J.H. Lee, J. Lloyd, P. Walter, S.G. Rane, Beneficial metabolic effects of a probiotic via butyrate-induced GLP-1 hormone secretion, J Biol Chem 288 (2013) 25088–25097. 101. V.A. Poroyko, A. Carreras, A. Khalyfa, A.A. Khalyfa, V. Leone, E. Peris, et al., Chronic sleep disruption alters gut microbiota, induces systemic and adipose tissue inflammation and insulin resistance in mice, Sci Rep 6 (1) (2016) 35405. 102. G.V. Bech-Nielsen, C.H. Hansen, M.R. Hufeldt, D.S. Nielsen, B. Aasted, F.K. Vogensen, et al., Manipulation of the gut microbiota in C57BL/6 mice changes glucose tolerance without affecting weight development and gut mucosal immunity, Res Vet Sci 92 (3) (2012) 501–508, 103. E. Sepp, H. Kolk, K. Lõivukene, M. Mikelsaar, Higher blood glucose level associated with body mass index and gut microbiota in elderly people. Higher blood glucose level associated with body mass index and gut microbiota in elderly people, Microb Ecol Health Dis 25 (2014) 22857. 104. N. Larsen, F.K. Vogensen, F.W. van den Berg, D.S. Nielsen, A.S. Andreasen, B.K. Pedersen, et al., Gut microbiota in human adults with type 2 diabetes differs from non-diabetic adults, PLoS One 5 (2) (2010) e9085. 105. H.K. Pedersen, V. Gudmundsdottir, H.B. Nielsen, T. Hyotylainen, T. Nielsen, B.A. Jensen, et al., Human gut microbes impact host serum metabolome and insulin sensitivity, Nature 535 (7612) (2016) 376–381. 106.X. Wu, C. Ma, L. Han, M. Nawaz, F. Gao, X. Zhang, et al., Molecular characterisation of the faecal microbiota in patients with type II diabetes, Curr Microbiol 61 (1) (2010) 69–78. 107.Q. Jia, L. Zhang, J.D. Zhang, F. Pei, S.W. Zhu, Q.H. Sun, et al., Fecal microbiota of diarrheapredominant irritable bowel syndrome patients causes hepatic inflammation of germ-free rats and berberine reverses it partially, Biomed Res Int 2019 (2019) 4530203. 108. H.T. Cui, Y.Z. Cai, L. Wang, B.T. Jia, J.C. Li, S.W. Zhao, et al., Berberine regulates Treg/Th17 balance to treat ulcerative colitis through modulating the gut microbiota in the colon, Front Pharmacol 9 (2018) 571.
Jo
ur
na
lP
re
-p
ro of
109. Y.N. Wang, X. Liu, Y. He, Q.M. Wang, X.L. Zhu, C.C. Wang, et al., Berberine may correct corticosteroid resistance induced by gut microbiota dysbiosis in immune thrombocytopenia, Blood 132 (Suppl. 1) (2018) 3769-3769. 110. J. Gong, M.L. Hu, Z.Y. Huang, K. Fang, D.K Wang, Q. J. Chen, et al., Berberine attenuates intestinal mucosal barrier dysfunction in type 2 diabetic rats, Front Pharmacol 8 (2017) 42. 111. M. Takahara, A. Takaki, S. Hiraoka, T. Adachi, Y. Shimomura, H. Matsushita, et al., Berberine improved experimental chronic colitis by regulating interferon-γ- and IL-17A-producing lamina propria CD4+ T cells through AMPK activation, Sci Rep 9 (1) (2019) 11934. 112. W. Jing, Y. Safarpour, T. Zhang, P. Guo, G. Chen, X. Wu, et al., Berberine upregulates Pglycoprotein in human Caco-2 cells and in an experimental model of colitis in the rat via activation of Nrf2-dependent mechanisms, J Pharmacol Exp Ther 366 (2) (2018) 332-340 113. S. Habtemariam, The Nrf2/HO-1 axis as targets for flavanones: Neuroprotection by pinocembrin, naringenin and eriodictyol, Oxid Med Cell Longev 2019 (2019) 4724920. 114. D. Li, J. Zheng, Y. Hu, H. Hou, S. Hao, N. Liu, et al., Amelioration of intestinal barrier dysfunction by berberine in the treatment of nonalcoholic fatty liver disease in rats, Pharmacogn Mag 13 (52) (2017) 677-682. 115. J. Shen, Z.X. Zuo, A.P. Mao, Effect of probiotics on inducing remission and maintaining therapy in ulcerative colitis, Crohn's disease, and pouchitis: meta-analysis of randomized controlled trials, Inflamm Bowel Dis 20 (1) (2014) 21-35. 116. H.M. Zhao, X.Y. Huang, Z.Q. Zuo, Q.H. Pan, M.Y. Ao, F. Zhou, et al., Probiotics increase T regulatory cells and reduce severity of experimental colitis in mice, World J Gastroenterol 19 (5) (2013) 742-749. 117. P.M. Smith, M.R. Howitt, N. Panikov, M. Michaud, C.A. Gallini, Y.M. Bohlooly, et al., The microbial metabolites, short-chain fatty acids, regulate colonic Treg cell homeostasis, Science 341 (2013) 569– 573. 118. M. Rajilić-Stojanović, E. Biagi, H.J. Heilig, K. Kajander, RA. Kekkonen, S. Tims, et al., Global and deep molecular analysis of microbiota signatures in fecal samples from patients with irritable bowel syndrome, Gastroenterology 141 (5) (2011) 1792–1801. 119. G.E. Buján, H.A. Serra, S.J. Molina, L.R. Guelman, Prevention of brain damage triggered by alcohol consumption during adolescence: Focus on oxidative stress, Curr Pharm Des (2019) doi: 10.2174/1381612825666191209121735 120. H.R. Sadeghnia, M. Kolangikhah, E. Asadpour, F. Forouzanfar, H. Hosseinzadeh, Berberine protects against glutamate-induced oxidative stress and apoptosis in PC12 and N2a cells, Iran J Basic Med Sci 20 (5) (2017) 594-603. 121. S.N. Maleki, N. Aboutaleb, F. Souri, Berberine confers neuroprotection in coping with focal cerebral ischemia by targeting inflammatory cytokines, J Chem Neuroanat 87 (2018) 54-59. 122. J.S. de Oliveira, F.H. Abdalla, G.L. Dornelles, S.A. Adefegha, T.V. Palma, C. Signor, et al., Berberine protects against memory impairment and anxiogenic-like behavior in rats submitted to sporadic Alzheimer's-like dementia: Involvement of acetylcholinesterase and cell death, Neurotoxicology 57 (2016) 241-250. 123. N.N. Yuan, C.Z. Cai, M.Y. Wu, H.X. Su, M. Li, J.H. Lu, Neuroprotective effects of berberine in animal models of Alzheimer's disease: a systematic review of pre-clinical studies, BMC Complement Altern Med 19 (1) (2019) 109. 124. S. Mehrzadi, I. Fatemi, M. Esmaeilizadeh, H. Ghaznavi, H. Kalantar, M. Goudarzi, Hepatoprotective effect of berberine against methotrexate induced liver toxicity in rats, Biomed. Pharmacother 97 (2018) 233-239. 125. Z. Zhao, Q. Wei, W. Hua, Y. Liu, X. Liu, Y. Zhu, Hepatoprotective effects of berberine on acetaminophen-induced hepatotoxicity in mice, Biomed Pharmacother 103 (2018) 1319-1326. 126. Y. Qing, X. Dong, L. Hongli, L. Yanhui, Berberine promoted myocardial protection of postoperative patients through regulating myocardial autophagy, Biomed Pharmacother 105 (2018) 1050-1053.
Jo
ur
na
lP
re
-p
ro of
127. Y. Yu, M. Zhang, Y. Hu, Y. Zhao, F. Teng, X. Lv, et al., Increased Bioavailable Berberine Protects Against Myocardial Ischemia Reperfusion Injury Through Attenuation of NFκB and JNK Signaling Pathways, Int Heart J 59 (6) (2018) 1378-1388. 128. G.L. Zhao, L.M. Yu, W.L. Gao, W.X. Duan, B. Jiang, X.D. Liu, et al., Berberine protects rat heart from ischemia/reperfusion injury via activating JAK2/STAT3 signaling and attenuating endoplasmic reticulum stress, Acta Pharmacol Sin 37 (3) (2016) 354-367 129. R. Domitrović, O. Cvijanović, E. Pernjak-Pugel, M. Skoda, L. Mikelić, Z. Crnčević-Orlić, Berberine exerts nephroprotective effect against cisplatin-induced kidney damage through inhibition of oxidative/nitrosative stress, inflammation, autophagy and apoptosis, Food Chem Toxicol 62 (2013) 397-406. 130. P. Hasanein, H. Riahi, Preventive use of berberine in inhibition of lead-induced renal injury in rats, Environ Sci Pollut Res Int 25 (5) (2018) 4896-4903. 131.C.G. Guan, S.M. Qiao, Q. Lv, N. Cao, K. Wang, Y. Dai, et al., Orally administered berberine ameliorates bleomycin-induced pulmonary fibrosis in mice through promoting activation of PPARgamma and subsequent expression of HGF in colons, Toxicol Appl Pharmacol 343 (2018) 1-15. 132.H.X. Liu, R. Keane, L. Sheng, Y.J. Wan, Implications of microbiota and bile acid in liver injury and regeneration, J Hepatol 63 (6) (2015) 1502–1510. 133.Y. Chen, F. Yang, H. Lu, B. Wang, Y. Chen, D. Lei, et al., Characterization of fecal microbial communities in patients with liver cirrhosis, Hepatology 54 (2) (2011) 562–572. 134.C.J. Qin, H.L. Zhang, L.H. Zhao, M. Zeng, W.J. Huang, G.B. Fu, et al., Microbiota transplantation reveals beneficial impact of berberine on hepatotoxicity by improving gut homeostasis, Sci ChinaLife Sci 61 (12) (2018) 1537-1544. 135. Q. Jia, L. Zhang, J.D. Zhang, S.W. Zhu, Q.H. Sun, L.P. Duan, Berberine patrtyially revised the effects of IBS-D patients fecal microbhiota induced hepatic inflammation in germ-free rats, Gastroenterology 154 (6) (2018) S1126-S1126. 136. X. Jia, L. Jia, L. Mo, S. Yuan, X. Zheng, J. He, et al., Berberine ameliorates periodontal bone loss by regulating gut microbiota, J Dent Res 98 (1) (2019) 107-116. 137. H. Wang, L. Guan, J. Li, M. Lai, X. Wen, The effects of berberine on the gut microbiota in Apc min/+ mice fed with a high fat diet, Molecules 23 (9) (2018) pii: E2298. 138. R. Gao, C. Kong, H. Li, L. Huang, X. Qu, N. Qin, et al., Dysbiosis signature of mycobiota in colon polyp and colorectal cancer, Eur J Clin Microbiol Infect Dis 36 (12) (2017) 2457-2468. 139. Y.N. Yu, TC. Yu, H.J. Zhao, T.T. Sun, H.M. Chen, H.Y. Chen, et al., Berberine may rescue Fusobacterium nucleatum-induced colorectal tumorigenesis by modulating the tumor microenvironment, Oncotarget 6 (31) (2015) 32013-32026. 140. Y. Sun, W. Wang, Y. Tong, Berberine inhibits proliferative ability of breast cancer Cells by reducing metadherin, Med Sci Monit 25 (2019) 9058-9066. 141. C. Gong, X. Hu, Y. Xu, J. Yang, L. Zong C. Wang et al., Berberine inhibits proliferation and migration of colorectal cancer cells by downregulation of GRP78, Anticancer Drugs (2019) doi: 10.1097/CAD.0000000000000835. 142. Q.Q. Chen, J.M. Shi, Z. Ding, Q. Xia, T.S. Zheng, Y.B. Ren, et al., Berberine induces apoptosis in non-small-cell lung cancer cells by upregulating miR-19a targeting tissue factor, Cancer Manag Res 11 (2019) 9005-9015. 143. F. Li, X. Dong, P. Lin, J. Jiang, Regulation of Akt/FoxO3a/Skp2 axis is critically involved in berberine-induced cell cycle arrest in hepatocellular carcinoma cells, Int J Mol Sci 19 (2) (2018) pii: E327. 144. S. Okubo, T. Uto, A. Goto, H. Tanaka, T. Nishioku, K. Yamada, et al., Berberine induces apoptotic cell death via activation of caspase-3 and -8 in HL-60 human leukemia cells: Nuclear localization and structure-activity relationships, Am J Chin Med 45 (7) (2017) 1497-1511. 145. Q. Hu, L. Li, X. Zou, L. Xu, P. Yi, Berberine attenuated proliferation, invasion and migration by targeting the AMPK/HNF4α/WNT5A pathway in gastric carcinoma, Front Pharmacol 9 (2018) 1150.
Jo
ur
na
lP
re
-p
ro of
146. Y. Kou, L. Li, H. Li, Y. Tan, B. Li, K. Wang, et al., Berberine suppressed epithelial mesenchymal transition through cross-talk regulation of PI3K/AKT and RARα/RARβ in melanoma cells, Biochem Biophys Res Commun 479 (2) (2016) 290-296. 147. L. Li, X. Wang, R. Sharvan, J. Gao, S. Qu, Berberine could inhibit thyroid carcinoma cells by inducing mitochondrial apoptosis, G0/G1 cell cycle arrest and suppressing migration via PI3KAKT and MAPK signaling pathways, Biomed Pharmacother 95 (2017) 1225-1231. 148. C.Y. Lin, P.L. Hsieh, Y.W. Liao, C.Y. Peng, M.Y. Lu, C.H. Yang, et al., Berberine-targeted miR-21 chemosensitizes oral carcinomas stem cells, Oncotarget 8 (46) (2017) 80900-80908. 149. Wang, Y. Zhang, S. Berberine suppresses growth and metastasis of endometrial cancer cells via miR-101/COX-2, Biomed Pharmacother 103 (2018) 1287-1293. 150. X. Liu, Q. Ji, N. Ye, H. Sui, L. Zhou, H. Zhu, et al., Berberine inhibits invasion and metastasis of colorectal cancer cells via COX-2/PGE2 mediated JAK2/STAT3 signaling pathway, PLoS One 10 (5) (2015) e0123478. 151. C. Wen, L. Wu, L. Fu, X. Zhang, H. Zhou, Berberine enhances the anti-tumor activity of tamoxifen in drug-sensitive MCF-7 and drug-resistant MCF-7/TAM cells, Mol Med Rep 14 (3) (2016) 22502256. 152. L. Wang, D. Wei, X. Han, W. Zhang, C. Fan, J. Zhang, et al., The combinational effect of vincristine and berberine on growth inhibition and apoptosis induction in hepatoma cells, J Cell Biochem 115 (4) (2014) 721-730. 153. L. Liu, J. Fan, G. Ai, J. Liu, N. Luo, C. Li, et al., Berberine in combination with cisplatin induces necroptosis and apoptosis in ovarian cancer cells, Biol Res 52 (1) (2019) 37.
PII:
S1043-6618(20)30149-3
DOI:
https://doi.org/10.1016/j.phrs.2020.104722
Reference:
YPHRS 104722
To appear in:
Pharmacological Research
Received Date:
13 January 2020
Revised Date:
21 February 2020
Accepted Date:
23 February 2020
Please cite this article as: Habtemariam S, Berberine Pharmacology and the Gut Microbiota: A Hidden Therapeutic Link, Pharmacological Research (2020), doi: https://doi.org/10.1016/j.phrs.2020.104722
This is a PDF file of an article that has undergone enhancements after acceptance, such as the addition of a cover page and metadata, and formatting for readability, but it is not yet the definitive version of record. This version will undergo additional copyediting, typesetting and review before it is published in its final form, but we are providing this version to give early visibility of the article. Please note that, during the production process, errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain. © 2020 Published by Elsevier.
Berberine Pharmacology and the Gut Microbiota: A Hidden Therapeutic Link Solomon Habtemariam Pharmacognosy Research Laboratories & Herbal Analysis Services UK, University of Greenwich, ChathamMaritime, Kent ME4 4TB, UK; [email protected]; Tel.: +44-208-331-8302 Received: 26 November 2019; Accepted: 11 December 2019; Published: date
re
-p
ro of
Graphical abstract
Abstract
Jo
ur
na
lP
Berberine is a natural pentacyclic isoquinoline alkaloid that has been isolated as the principal component of many popular medicinal plants such as the genus Berberis, Coptis and Hydrastis. The multifunctional nature of berberine as a therapeutic agent is an attribute of its diverse effects on enzymes, receptors and cell signalling pathways. Through specific and general antioxidant and antiinflammatory mechanisms, its polypharmacology has been established. Intriguingly, this is despite the poor bioavailability of berberine in animal models and hence begging the question how it induces its reputed effects in vivo. A growing evidence now suggest the role of the gut microbiota, the so-called the hidden organ, as targets for the multifunctional role of berberine. Evidences are herein scrutinised to show that the structural and numerical changes in the gut microbiota under pathological conditions are reversed by berberine. Examples in the pharmacokinetics field, obesity, hyperlipidaemia, diabetes, cancer, inflammatory disease conditions, etc. are used to show the link between the gut microbiota and the polypharmacology of berberine. Keywords: Berberine, microbiota, diabetes, obesity, hyperlipidaemia, infection, inflammation, SCFA, Firmicutes-to-Bacteroidetes ratio.
1. Introduction
-p
ro of
Berberine (Figure 1) is a natural pentacyclic isoquinoline alkaloid which is abundantly found as a principal constituent of many medicinal plants. The classic examples of berberine sources are the stems and roots of Berberis species including B. aristata [1,2], B. darwinii [3,4], B. Petiolaris [5] and B. vulgaris [6]. These berberine-containing plants with high yield of up to 5% of their dry weight have been reported. Composition up to 8-9% berberine in the rhizomes of many medicinal plants have also been known with the most researched plants to date include Argemone mexicana, Coptis chinensis (Chinese goldthread), C. japonica, C. teeta, Eschscholzia californica and Hydrastis Canadensis or goldenseal, Mahonia aquifolium, Tinospora cordifolia, Xanthorhiza simplicissima, and Phellodendron amurense. One characteristic feature of berberine is its distinctive yellowish colour that gives the source plant materials their yellow to gold appearance (Figure 1).
re
Figure 1. The structure of berberine and its deep yellow colour.
Jo
ur
na
lP
In its chemically pure form, berberine is known to be first isolated from H. canadensis (goldenseal) in 1917 [7] but its use as a principal component of plants was dated to antiquity primarily as a dye (e.g., the textile industry) due to its deep yellow and yellow fluorescent characteristics. Its medicinal use was also dated for centuries as an active principle for numerous medicinal plants which are still in use to date including as ingredients of various food supplements. The pharmacology of berberine has been extensively studied and include anti-inflammatory [8,9], anticancer [10-12], antidiabetic [13-15], antiobesity and anti-hyperlipidaemic [14,16], cardioprotective [17,18] and spatial memory enhancement [19-21] effects. The plethora of pharmacological effects recorded for berberine attributes to some specific effects on enzymes, receptors and other biological targets along with other general effects such as antioxidant and anti-inflammatory properties. As with many natural products, the therapeutic potential of berberine could be explained by the polypharmacology principle of drug action [22] though research on the mechanisms of action that account to its diverse effects still continues. This article is designed to shade some light on the potential contribution of the gut microbiota to berberine’s multifunctional bioactivity.
2. Pharmacokinetics Even though berberine is a cationic alkaloid, its structure is by no means optimised for rapid absorption from the gut. It is sparingly soluble in water implying that it has poor intestinal absorption and/or bioavailability. In fact, the absolute bioavailability of berberine is far less than 1% given that even the absorbed berberine from the gut could be excreted back to the intestinal lumen through the action of P-glycoprotein. Chen et al. [23] reported absolute bioavailability from the oral route in rats as 0.68%, and as expected, inhibitors of P-glycoprotein could increase bioavailability from the intestine. Berberine absorption in rats could also be improved by up to 6-times by P-glycoprotein inhibitors
Jo
ur
na
lP
re
-p
ro of
suggesting the contribution of P-glycoprotein to the poor intestinal absorption of berberine [24]. An absolute oral bioavailability in rats of 0.36% has also been reported making intestinal first-pass elimination of berberine as the major barrier to its oral bioavailability [25]. With such poor degree of absorption from the gut, berberine ingested in hamsters is largely accumulated in the gut (not the circulation) and its bioavailability through intraperitoneal route is much better than the oral/intragastric route [26]. Based on HPLC analysis of human plasma following berberine oral dose, the absolute bioavailability was considered extremely low with the maximum plasma concentration of about 0.4 ng/ml obtained following 400 mg oral dose [27]. Despite all these, berberine has been shown to induce pharmacological effects in a plethora of animal models. Once absorbed, berberine has also shown to be distributed into all major organs with the highest amount obtained in the liver and readily excreted via the urine [28]. One of the emerging links between the expected poor bioavailability of berberine and its pharmacology is the gut microbiota that modulate both the pharmacokinetics profile and its biological effects. In beagle dogs, for example, oral administration of berberine leads to changes in the intestinal bacterial composition and butyrate (a product of bacteria) level in the gut [29]. In this case, treatment with berberine for seven days could increase the abundance of butyrate- and the nitroreductases-producing bacteria though the plasma level of berberine was still very low with the maximum level detected following an oral administration of 50 mg/kg was 37 ng/ml [29]. Earlier studies have also shown that berberine could enhance the oral bioavailability of other drugs. The bioavailability of ciclosporin A, for example, was shown to be augmented in healthy human volunteers resulting from the suspected decrease in liver and intestinal metabolism through inhibition of CYP3A4 [30]. Recent studies however pinpoint the role of the gut microbiota as a major target for modulation of drug pharmacokinetics by berberine. Accordingly, the pharmacokinetics interaction of berberine and metformin include the berberine-induced increase in metformin level coupled with decreased metformin degradation by rat and human intestinal bacteria [31]. Guo et al. [32] further showed that oral administration of berberine in mice could lead to increased expression of bile acidssynthetic enzymes (Cyp7a1 and 8b1) and uptake transporter (Ntcp) in the liver while the level of Bacteroides in the terminal ileum and large bowel were enhanced. An inspiring research on the role of the gut microbiota in the pharmacokinetics of berberine and potential variations between Chinese and Africans has been investigated by Alioga et al. [33]. The study revealed a higher abundance of the genera Prevotella, Bacteroides, and Megamonas (34.22, 13.88, and 10.68%, respectively) in the Chinese than the Africans subjects with more extensive metabolism was observed in the Chinese group. This study highlights that inter-individual and inter-racial differences in drug metabolism could be linked to variations in the gut microbiota. Dietary habits and antibiotics therapy are also likely to affect the state of the individual’s response in the pharmacokinetics and pharmacology of berberine. One mechanism for enhancing the biological activity of berberine by the gut microbiota lies in their ability to convert it into a better absorbable form, dihydroberberine. Feng et al. [34] reported a 5-fold increase in intestinal absorption rate for dihydroberberine than berberine in animals. In mice, the microbiota could reduce berberine to dihydroberberine which is absorbed into intestinal tissue and subsequently oxidised back to berberine to enter the blood stream. This process too could be ameliorated by treatment with antibiotics [34]. The dual effect of berberine in its pharmacology either by enhancing the gut microbiota or through its own specific mechanism of action was noted by the study of Wang et al. [35]. They have shown that some of the effect of berberine could be attributed to the increased butyrate production in the gut and increased abundance of such bacteria which has profound effect on blood lipid and glucose levels. The mechanism of butyrate itself on blood level of glucose and lipids was however different begging into a question of multiple mechanisms of action. The role of the gut microbiota as mediators of berberine’s polypharmacology is detailed further in the following sections. 3.
General effect on the gut microbiota
re
-p
ro of
Although the direct antibacterial effect of berberine in vitro is somehow weak, the compound is widely known as an antibacterial agent including in vivo. Not surprisingly, one of its known mechanism in ameliorating intestinal inflammation in humans is through direct antibacterial action [36]. This includes effects against Escherichia coli in vitro [37,38]; Clostridium difficile-induced intestinal injury model in mice [39] and anti-diarrhoeal effect in human [40]. The most important function of berberine related to the present communication is its ability to modify the composition of the gut microbiota. Earlier studies have shown that berberine can induce cell death in harmful gut bacteria while enhancing the composition of beneficial bacteria including Bifidobacterium adolescentis and Lactobacillus acidophilus [41,42]. The mechanism of berberine in modifying diseases is thus somehow similar with those of probiotics [43-46]. Hence, under disease conditions such as colitis, inflammatory bowel disease (IBD) or related pathologies associated with gut inflammation, berberine can reverse the increased prevalence of harmful bacteria such as E. coli and enterococci bacteria and the pathology-induced decreased Lactobacilli and Bifidobacteria. The mild diarrhoea induction under clinical condition by berberine is also shown to be coupled with gut microbiota dysbiosis such as increased abundances of the families Porphyromonadaceae and Prevotellaceae as well as the genera of Parabacteroides, Prevotellaceae_UCG-001 and Prevotellaceae_NK3B31_group [47]. Analysis of microbiota in the gut of broilers under high stocking density has further shown that treatment with berberine could lower the level of E. coli while increasing Lactobacillus in the cecum [48]. Most of the experiments conducted on berberine discussed in the following sections are based on changes on the profile of the gut microbiota population. While the composition of the human gut microbiota could change with diet and many other factors, studies on the bacterial 16S rRNA gene sequences from the faecal microbiota of humans and 59 other mammalian species have shown the prevalent groups as Firmicutes (65.7%) and to the Bacteroidetes (16.3%) and small proportion of Proteobacteria (8.8%), Actinobacteria (4.7%), Verrucomicrobia (2.2%), Fusobacteria (0.67%), and others [49]. The composition of these gut microbiota under pathological condition and their modulation by berberine is worth further scrutiny (see the following sections).
lP
3.1. Anti-obesity and antihyperlipidemic effects through regulation of the gut microbiota
Jo
ur
na
The antiobesity potential of berberine has been demonstrated in numerous experimental models. Through the AMP-Activated Protein Kinase (AMPK)-dependent and independent mechanisms, berberine can inhibit adipogenesis in experimental animals [50]. In obese mice, berberine administered through peripheral or central route can lower liver weight, hepatic and plasma triglycerides (TGs), and cholesterol contents by promoting AMPK activity and fatty acid oxidation and modulation of expression of genes involved in lipid metabolism. Some of the effects of berberine in obesity could be linked to its ability to modulation of microRNA (miRNA) as shown from its inhibitory effect on 3T3-L1 adipocytes cell differentiation and reduction of TGs contents via increased mRNA expression levels of miRNA-27a and miRNA-27b [51]. This in turn is linked to the negative regulation of the peroxisome proliferator-activated receptors (PPAR)-γ by these miRNA (miRNA-27a). Adipocyte differentiation has also been widely reported as a mechanism for the antiobesity effect of berberine through various distinct mechanisms including suppression of galectin-3 in mouse primary preadipocytes isolated from epididymal white adipose tissues [52]. It also suppresses the cAMPresponse element-binding protein (CREB) phosphorylation and CCAAT-enhancer-binding proteinβ(C/EBPβ) expression at the early stage of 3T3-L1 preadipocyte differentiation [53]. Berberine could also enhance thermogenesis in white adipose tissues [54]. Berberine further regulates lipid metabolism by upregulating hepatic low-density lipoprotein (LDL) receptors through the AMPK-dependent Raf-1 activation pathway [55]. One of the best researched experimental models for the antiobesity effect of berberine is the highfat diet-induced obesity in mice where it has been shown to inhibit adipogenesis [57]. The aniobesity (weight loss), lipid lowering effect of berberine as a function of TGs and cholesterol reduction have been demonstrated in both rats and humans [58]. Through both central and peripheral action that are
distinctly different from the statins, berberine is now known as a potent antiobesity and lipid lowering agent [59,60]. It is based on this plethora of evidences for berberine as weight, lipid and cholesterol lowering agent [26, 61-74] that its mechanism through modulation of the gut microbiota (Table 1) is scrutinised herein.
Jo
ur
na
lP
re
-p
ro of
Table 1. The antiobesity and antihyperlipidemic pharmacology of berberine via modulation of the gut microbiota Bioassay model Dosage Key finding References db/db mice 136.5 mg/kg, i.g. Increase SCFA content in faeces; modulate the Zhang et for 11 weeks ratio of Firmicutes-to-Bacteroidetes; increase al. [62] the proportions of Butyricimonas, Lactobacillus, Coprococcus, Ruminococcus, and Akkermansia; reduce the proportions of Prevotella and Proteus at the genus level. High-fat diet- Added to Increase the abundance of Akkermansia spp. Zhu et al. induced drinking water [63] atherosclerosis in (0.5 g/L) for 14 ApoE-/- mice weeks. High-fat diet- 50 mg/kg twice Enrich Firmicutes and Verrucomicrobia and Shi et al. induced weekly, i.g. for decrease Proteobacteria at the phylum level [64] atherosclerosis in 12 weeks when compared with the disease model. ApoE-/- mice Colorectal cancer Diet supplement Alter the structure of gut microbiota - inhibits Wang et al. development in with 500 ppm of the increase in Verrucomicrobia (phylum level); [65] Akkermansia and increase high-fat diet- berberine for 12 decrease Lachnospiraceae_incertae_ sedis (genus level); min/+ obese Apc weeks trends of increase in Bacteroidetes abundance; mice elevate some SCFAs-producing bacteria. High-fat diet- 100 mg/kg, p.o. Reverse the dysbiosis and a reduction in Sun et al. obese mice for 8 weeks SCFAs (butyric, acetic, propionic, isobutyric, [66] isovaleric, valeric acids), in the colon of obese mice; decrease the Firmicutes/Bacteroidetes ratio under obesity. High-fat diet 150 mg/kg, p.o. Reduce the richness and diversity of the gut Xu et al. obesity model in 6 weeks microbiota: increasing the abundance of [67] rats Fusobacteria and Proteobacteria, and decreasing the abundance of Firmicutes and Actinobacteria; no effect on the abundance of the Bacteroidetes phylum; At the genus level, those increased by berberine under obesity include Fusobacterium, Anaerostipes, Bacteroides and Phascolarctobacterium, Erysipelotrichaceae_Incertae_Sedis, Peptostreptococcaceae_Incertae_Sedis and Escherichia-Shigella; while those decreased include Roseburia, Allobaculum, Oscillibacter, Faecalibacterium, Prevotella Desulfovibrio, Coprococcus, Collinsella and Blautia. High-fat diet‐ 100 mg/kg, p.o. Increased berberine bioavailability correlate Wang et al. induced obese for 10 days in with increase in NR activity. [68] hamsters; animals; 500 mg
in
Sun et al. [69]
200 mg/kg, p.o. for 8 weeks
Reverse the decreased level of Bifidobacterum and Bacteroidete in obesity.
Cao et al. [70]
150 mg/kg containing a formulation with 24 mg/kg of oryzanol and 10 mg/kg of vitamin B6; p.o for 4 weeks 150 mg/kg, p.o. for 4 months
Enrich beneficial bacteria (e.g. Bacteroides, Blautia) and decrease the abundance of Escherichia at the genus level.
Li et al. [71]
ro of
Increase conjugated bile acids in serum and their excretion in faeces; inhibits BSH activity in gut microbiota.
Increase the Bacteroidetes-to-Firmicutes (B/F) ratio in obese rats; At the genus level those enriched include Bacteriodes (SCFAproducing) as Bacteriodetes and those suppressed (Firmicutes) include Dorea, Roseburia, and Blautia; others increased include Anaerofilum, Bilophila (SCFAproducing), and Desulfovibrio. Modulate the gut microbiota (increased the proportion of Firmicutes and reduce the proportion of Bacteroidetes); inhibits the 7αdehydroxylation conversion of cholic acid to deoxycholic acid (decreased elimination of bile acids in the gut). Similar effect for both drugs reduce diversity of gut microbiota; of the 134 OTUs identified, sixty were decreased by both drugs; increase the abundance of those belonging to putative SCFAs-producing bacteria (Allobaculum, Bacteriodes, Blautia, Butyricoccus and Phascolarctobacterium). Reduce bacterial diversity with selective enrichment of putative short-chain fatty acid (SCFAs)-producing bacteria (Blautia and Allobaculum); increase elevations of faecal SCFAs concentration; bacterial list on the increase are Allobaculum, Bacteroides, Blautia, Butyricicoccus, Lactobacillus,
Sun et al. [72]
na
100 mg/kg, i.g. for 2 weeks
ur
High-fat dietinduced hyperlipidaemia model in hamster
lP
re
High-fat-fed obese rats
once daily humans
-p
Hyperlipidaemic and normal subjects High-fat dietinduced obesity in wild type (WT) and FXR knockout (FXRint-/) mice High-fat dietinduced Steatohepatitis and dysbiosis of the gut microbiota in mice High-fat dietinduced hyperlipidaemia in rats
Jo
High-fat dietinduced obesity in rats
High-fat diet-fed obese rats
100 or 200 mg/kg berberine or metformin, i.g. for 8 weeks
100 mg/kg, p.o. for 8 weeks
Gu et al. [26]
Zhang al. [73]
et
Zhang al. [74]
et
Phascolarctobacterium, Parasutterella, Dorea, Clostridium XVIII and Fusobacterium and Klebsiella; those suppressed include Clostridium XlVa, Flavonifractor, Lachnospiracea_incertae_sedis, Roseburia and Clostridium XI. Abbreviations: BSH, bile salt hydrolase; NR, nitroreductases; OTUs, operational taxonomic units; SCFAs, short chain fatty acids.
Jo
ur
na
lP
re
-p
ro of
The association between obesity and change in the gut microbiota has been shown to be the key to the effect of berberine as antiobesity agent. This in a way is also linked to the differential pharmacokinetics of berberine under normal and disease states in the gut microbiota. Wang et al. [68] have shown that berberine is more bioavailable in obese than lean animals owing to the differential microbiota composition. By using the high-fat diet-induced non-alcoholic steatohepatitis model in mice, Cao et al. [70] investigated the effect of berberine on the caecal content of proportions of Bacteroidetes, Firmicutes, Bifidobacteria and Lactobacillus species. The antiobesity effect of berberine in this model was established through the significant reduction in body weight and serum lipids (TG and TC). As a link between obesity and diabetes (see, Section 3.2), the anti-inflammatory mechanism of berberine in this model was also evident given the reduction in the level of proinflammatory cytokines such as IL-1, IL-6 and TNF-α which are known to be the major link between obesity and diabetes. Beyond amelioration of obesity and associated disease markers, berberine could reverse the diseaseassociated suppression of the Lactobacillus and Bifidobacterium levels. The obesity-mediated alteration of the microbial ecology [75] is thus a target for berberine. A similar experiment on the high-fat diet-induced hyperlipidaemia model was conducted in hamsters where berberine treatment effectively showed antihypercholesteraemic effect [26]. This is despite the poor pharmacokinetic profile of berberine through the oral route of administration discussed in Section 2. More importantly, treatment with berberine through an oral route could modulate the proportion of Firmicutes and Bacteroidetes in hypercholesteraemic hamsters. As a note of the Firmicutes-to-Bacteroideteratio (F/B) ratio, it was 1.43 in health animals while it was 0.95 in hypercholesteraemic hamsters before berberine treatment increased it to 1.6 [26]. In the hypocholestrolaemic activity study in rats, Li et al. [71] also demonstrated the ameliorative effects of changes in the serum, urine, liver and faecal metabolites. They noted a higher abundance of Bacteroides, Parabacteroides and Blautia after berberine treatment with a concomitant decrease in the genus Escherichia. The taxon-based analysis by Sun et al. [69,72] further showed that Firmicutes, Bacteroidetes, and Proteobacteria were the major phyla of faecal microbiota in rats while after high-fat-induced obesity, berberine could induce a decline in Firmicutes abundance and a moderately increase in Bacteroidetes ratios. Hence, a higher Bacteroidetes-to-Firmicutes (B/F) ratio was observed in obese animals treated by berberine. They also noted the enriching effects of berberine on Bacteroidaceae and Rikenellaceae families; both belonging to the Bacteroidetes phylum. In contrast, the elevated abundances of Christensenellaceae, Dehalobacteriaceae, Erysipelotrichaceae and Peptococcaceae (all belonging to the Firmicutes phylum) in in obese animals declined after treatment with berberine. This was in addition to the increased Alcaligenaceae (Proteobacteria Phylum) in obese animals after treatment with berberine. The effect of berberine as a lipid-lowering agent has been shown to be linked to the gut via modulation of the turnover of bile acids and subsequently the ileal Farnesoid X receptor (FXR) signalling pathway [69]. As receptors for bile acids and regulator of bile acid and their transporters synthesis, the FXR has close working relationship with the gut microbiota. For example, the gut microbiota is the source of the enzyme bile salt hydrolase (BSH) that hydrolyse bile acids conjugates [76]. Hence, the effect of berberine on FXR signalling is similar with the known effect of antibiotics and probiotics in lipid metabolism via microbial remodelling [77,78].
The study by Sun et al. [66] tried to determine the relationship between the bacteria-derived SCFAs with obesity-related markers. They have shown that the level of six types of SCFAs (butyric acid, acetic acid, propionic acid, isobutyric acid, isovaleric acid, and valeric acid) were reduced in obese mice with the most pronounced effect observed in butyric acid. The partial blockage of obesity and diabetes (see, Section 3.2) was associated with modulation of the gut microbiota (Table 1). Once again, Firmicutes and Bacteroidetes are the most abundant bacteria in the gut microflora at the phylum level but the general trend was for Firmicutes to increase and Bacteroidetes to decrease under obesity. Under this condition, the ratio of F/B in obese animals could be increased by up to 10-folds in obese mice which was suppressed by berberine treatment. At the genus level, berberine could also reverse the relative abundance of Clostridiales.g and Oscillospira under obesity condition [66].
Jo
ur
na
lP
re
-p
ro of
In obese animals, berberine has been shown to suppress weight gain along with critical effect on the gut microbiota. Zhang et al. [73], for example have shown treatment of high-fat diet-induced obese animals both by berberine and metformin led to an increase in the total relative abundance in 7 operational taxonomic units (OTUs) to 10–20% from less than 2%. Of the 7 OTUs, six were shown to be major SCFA-producing bacteria such as Blautia, Bacteriodes, Butyricoccus and Phascolarctobacterium. Unlike other studies, however, they reported that neither an increase of the F/B ratio after drug treatments nor any correlation between F/B ratio and body weight or adiposity index. The most recent experiment by Zhang et al. [62] using the db/db mouse model of obesity, diabetes, and dyslipidaemia showed similar effects (Table 1) where the microbiota modulation by berberine was shown to be involved in its antiobesity effect. The study by Zhang et al. [74] on the effect of berberine on obesity through the gut microbiota was among the most comprehensive since they included 3764 OTUs, contributing to 53.51% of all reads for the he most abundant phyla Firmicutes and 1753 OTUs, contributing to 34.83% of all reads for Bacteroidetes. Other phyla included the Proteobacteria (341 OTUs, contributing to 6.22% of all reads), and Actinobacteria (139 OTUs, contributing to 1.15% of all reads). While higher abundances of the phyla Actinobacteria and Verrucomicrobia were observed in the high-fat diet-obese group than normal animals, and trend was shown to be completely reversed by berberine. They also reported that berberine treatment could increase the faecal concentration of total SCFAs, particularly acetic acid and propionic acid, in obese rats. The trend of change for butyric acid was not significant suggesting some discrepancies among the different studies on the role of individual SCFA in obesity-related pathology. In the study of high-fat diet-induced atherosclerosis development in mice, Shi et al. [64] assessed the effect of berberine in the gut microbiota composition, which was dominated by the Firmicutes and Bacteroidetes, followed by Proteobacteria and Verrucomicrobia at the phyla level. The Firmicutes and Verrucomicrobia appeared to be enriched by berberine treatment while the level of Proteobacteria were suppressed when compared with the disease-model groups. The reduction of atherosclerosis score and inflammation by berberine in high-fat diet-induced atherosclerosis in ApoE-/- mice was similarly coupled with microbiota modulation by berberine: increase the abundance of Akkermansia spp. [63]. Hence, there seem to be an overwhelming evidence to suggest that the effect of berberine in obesity, hyperlipidaemia and cholesterol-induced pathologies could be in part linked to modulation of the gut microbiota. More evidences in other pathologies are discussed in the following sections.
3.2. Antidiabetic effects through gut microbiota regulation The efficacy of berberine in type-2 diabetes (T2D) patients have been effectively demonstrated in recent years [79-81]. Its direct effect on increasing the expression level of insulin receptors and to lower blood glucose level in T2D patients have been shown [82]. Hence, berberine is now known to act as antidiabetic agent through modulation of insulin signalling [83]. It is also often regarded as an insulin sensitizing and insulinotropic agent [84]. Meta-analysis of randomised clinical trial data further suggests the antidiabetic potential of berberine for diabetes [85]. In addition to the effect of berberine
in obesity and hyperlipidaemia states discussed in the previous section, it also acts through several other mechanisms including glucagon-like peptide-1 (GLP-1) release [13,86]. Through activation of the AMPK, berberine can also ameliorate the T2D-associated cardiac dysfunction both in cellular and animal models [87]. In high-fat diet-induced obese mice model and macrophages and 3T3-L1 adipocytes in vitro, berberine could ameliorate inflammation, improve glucose tolerance, reduce the increased expressions of inflammatory mediators (TNF-α, IL-6 and MCP-1) and ameliorate the phosphorylation of JNK and IKKβ, the expression of NF-κB p65 IRS-1 (Ser307). Furthermore, berberine inhibits the phosphorylation of IRS-1 (Ser307) while increasing the phosphorylation of AKT (Ser473) in adipose tissue and cultured adipocytes [88]. In addition, berberine can lower glucose level by inducing glycolysis [89] as well as inhibition of gluconeogenesis [90].
ro of
The antidiabetic effect of berberine through its modulatory effect on the gut microbiota is summarised in Table 2 [56,61,62,67,70,74,91-97]. Some of these effects are similar with what is already known for the well-known antidiabetic agent, metformin, which has a profound effect on the microbial diversity (decrease) in high-fat diet-fed mice even more than in lean mice [98]. Table 2. Antidiabetic effect of berberine associated with alteration of microbiota.
In vivo - 200 mg/kg, p.o. for 10 weeks; in vitro - 10, 50 or 100 µM
na In vivo at 100 mg/kg for 5 days; or in vitro on isolated mouse cecal bacteria at 0.1, 1, and 10 mg/mL for 4 hours in an anaerobic chamber
Jo
ur
In vivo in mice or direct effect on bacteria in vitro
db/db mice
136.5 mg/kg metformin 113.75 mg/kg for 11 weeks
or at i.g
References Pan et al. [91]
-p
High-fat diet-fed mice; hepatocytes and 3T3-L1 adipocytes
Key finding Increase the composition of gut microbiota - the enriched OTUs mainly belong to Firmicutes; ameliorate the changes in dominance of Proteobacteria, Planctomycetes, Bacteroidetes, and Firmicutes; alter the decrease in the ratio of Firmicutes to Bacteroidetes; 32 berberine-OTUs negatively correlate with glucose level. Decrease the relative abundance of BCAA-producing bacteria (order Clostridiales; family Streptococcaceae and genera Streptococcus; Clostridiaceae, and Prevotellaceae (genera Prevotella); increased in abundance include Akkermansia (genus of the phylum Verrucomicrobia). In vivo - Alter intestinal bacteria by reducing Firmicutes and Clostridium cluster XIVa and BSH activity; In vitro alter bacterial physiology and bacterial community composition and function (reduce BSH-expressing bacteria like Clostridium spp); no effect on Bacteroidetes but reduce the Firmicutes/Bacteroidetes ratio. Increase SCFA content in faeces; modulate the ratio of Firmicutes-toBacteroidetes; increase the proportions of Butyricimonas, Lactobacillus, Coprococcus, Ruminococcus, and Akkermansia; reduce the proportions of Prevotella and Proteus.
re
Dosage Diet supplementation at a dose of 30 mg/Kg
lP
Bioassay model Grass carp (Ctenopharyngodon idellus)
Yue [92]
et
al.
Tian et al. [93]
Zhang et al. [62]
200 mg/kg, p.o. for 8 weeks
High-fat obese mice
100 mg/kg, p.o. for 8 weeks; cellular model of CI-H716 cells treated with palmitic acid – berberine at 100 µM 150 mg/kg, p.o. 6 weeks
300 mg berberine three times daily, 0.5 h after each major meal for 8 weeks
200 mg/kg, p.o. for 8 weeks
ur
Patients aged 18-65 years with newly diagnosed T2D with (BMI) > 25 kg/m2 before and 8 weeks after treatment High-fat diet-dietinduced Steatohepatitis and dysbiosis of the gut microbiota in mice High-fat-fed obese rats STZ combined with high-fat diet in Rats High-fat diet-fed obese rats
Reduce the richness and diversity of the gut microbiota; increase the abundance of Fusobacteria and Proteobacteria, and decrease the abundance of Firmicutes and Actinobacteria; no effect on the abundance of the Bacteroidetes phylum. Increase in total Bifidobacterium level, Bifidobacterium longum, Bifidobacterium breve, Bifidobacterium adolescentis, and Bifidobacterium infantis in good correlation (except Bifidobacterium breve) with TNF-α and LPS levels.
Xu et al. [67]
Restore the relative level Bifidobacterium and Bacteroidate.
Cao [70]
150 mg/kg, p.o. for 4 months 100 mg/kg, p.o. for 2 weeks
of
Increase the Bacteroidetes-to-Firmicutes ratio in obese rats; see details in Table 1. Decrease in plasma LPS level by increasing tight junction protein (ZO1) expression. 100 mg/kg, p.o. for Reduce bacterial diversity while 8 weeks selectively enriching putative SCFAproducing bacteria (Blautia and Allobaculum); increase elevations of faecal SCFA concentration; see details in Table 1. Abbreviations: LPS, lipopolysaccharide; TNF-α tumour necrosis factor-α.
Jo
Liu et al. [95]
Sun [66]
et
al.
Chen et al. [96]
lP
High-fat diet obesity model in rats
na
diet-
Cui et al. [94]
ro of
High-fat diet obesity-induced diabetes in rats
Increase the populations of Bacteroidetes, Clostridia, Lactobacillales, Prevotellaceae, and Alloprevotella; reduce those of Bacteroidales, Lachnospiraceae, Rikenellaceae, and Desulfovibrio. Reverse the obesity-induced change in the gut microbiota composition – ameliorate the reduction in protective bacteria like Bifidobacterium and the increased gram negative bacteria like Escherichia coli; ameliorate the increased LPS release into plasma. Modulate the changes in dysbiosis and the diabetes-associated reduction in SCFAs in the colon of obese mice (see Table 1)
-p
500 mg/kg, i.g. for 4 weeks
re
STZ-induced diabetic rats under high-fat, highsucrose diet
et
al.
Sun et al. [72] Shan et al. [97] Zhang et al. [74]
Jo
ur
na
lP
re
-p
ro of
In addition to the antiobesity and lipid lowering effect of berberine in the high-fat diet-induced non-alcoholic steatohepatitis model in mice (see, Section 3.1), Cao et al. [70] have shown a reduction in fasting blood glucose (FBG), insulin, and homeostasis model assessment of insulin resistance (HOMAIR) through alteration of the gut microbiota (Table 2). The link between diabetes and obesity being proinflammatyory cytokines and/or inflammation, the alteration of the structure and abundance of the microbiota in the gut was also associated with the observed anti-inflammatory effect. Moreover, berberine ameliorated the morphological and biochemical (ALT and AST) disease markers while the disease-associated suppression of Lactobacillus and Bifidobacterium levels were reversed. The effect of berberine in reversing the suppressed level of SCFAs in obese mice and increasing the ratio of F/B was coupled with its antidiabetic effect (Sun et al. [66]). In this connection, the more pronounced effect of berberine on butyric acid level was consistent with the effect of butyric acid on improvement of insulin sensitivity and increased energy expenditure in mice [99]. As with the antiobesity effect, the antidiabetic effect of probiotics has been shown to be mediated through butyrateinduced mechanism such as increased GLP-1 release [100]. The effect of berberine on diabetes, obesity, inflammation and microbiota modulation was also similar with metformin when assessed in the db/db mouse model of diabetes [62]. Chen et al. [96] studied the effect of berberine in newly diagnosed T2D and overweight patients. Although, the microbiota population studied was limited to the genus Bifidobacterium, four species (B. longum, B. breve, B. infantis and B. adolescentis) appeared to be enriched after berberine treatment. Moreover, the observed change in these group of bacteria, except for B. breve, were positively correlated with the reduction in the TNF-α and LPS levels induced by berberine. Hence, both the antidiabetic and antiobesity potentials of berberine are somehow linked to its anti-inflammatory effect which were all intern linked to changes in the microbiota population of the Bifidobacterium species. Cui et al. [94] recorded that several biochemical and morphological markers of diabetes could be suppressed by berberine (Table 2). These include increased level of antioxidants, insulin and GLP-1 together with reduction in the level of plasma glucose, lipids and insulin resistance. Along with inhibition of gluconeogenesis and enhanced glycolysis that all confer antidiabetic effect, there was an increase in the populations of Bacteroidetes, Clostridia, Lactobacillales, Prevotellaceae, and Alloprevotella while those of Bacteroidales, Lachnospiraceae, Rikenellaceae, and Desulfovibrio were reduced. They also reported the ratios of F/B in the normal, T2D, and berberine groups were 0.54, 1.09, and 0.73, respectively. Hence, the structural changes along with the F/B ratio in the intestines appears to be positively correlated with blood glucose concentrations in diabetic rats. The study by Cui et al. [94] further established that the Clostridiales and Bacteroidales were the dominant orders in the intestines of all treatment groups in rats: while the relative abundances of Clostridiales (35.91%) and Lactobacillales (2.46%) were lower than that of Bacteroidales (47.31%) in the T2D group, with berberine tended to abolish this order. The study by Liu et al. [95] did not find a significant effect on body weight, visceral fat mass or the visceral fat to body weight ratio following treatment of high-fat-fed obese rats with berberine. They have shown however that the inflammatory components of diabetes were ameliorated along with improvement in insulin resistance as well as insulin receptor and insulin receptor substrate-1 expression in the liver. These effects along with pathological markers such as hepatic steatosis was shown to be ameliorated by berberine together with reversal of the obesity-induced alteration of the gut microbiota composition. In particular, the reduction in protective bacteria like Bifidobacterium and increased gram-negative bacteria like E. coli in obesity and berberine’s ability to reverse this trend was suggested as potential mechanism for its antidiabetic properties. A randomized, double-blind and Placebo-controlled Study under the title “Effectiveness and Safety of Berberine Hydrochloride and Bifidobacterium in People with Abnormal Glucose Level” were conducted in China with 300 participants of newly diagnosed patients with pre-diabetes or T2D. Given Bifidobacterium, as a known probiotic that can modulate the gut microbiota and improve glucose and
-p
ro of
lipid metabolism in animal experiments, the 16-weeks study was designed to investigate the link between the antihyperglycaemic effect of berberine tablets by its own and in combination with bifidobacterium mimetic capsules. The primary outcome is the absolute value of fasting plasma glucose and the results are still awaiting. In fish, the study by Pan et al. [91] revealed that the effect of berberine in glucose level of the serum was associated with structural modulation of the gut microbiota. The enriched OTUs mainly belonging to Firmicutes altered to the dominance of Proteobacteria, Planctomycetes, Bacteroidetes, and Firmicutes during and after berberine feeding; decrease the ratio of F/B; 32 berberine-OTUs were significantly negative correlated with glucose level. Readers should bear in mind that this change was on healthy animals and the trend could be different in diabetic animals. The study by Shan et al. [97] did not directly aimed at the microbiota level but they have shown that fasting insulin, insulin resistance index, plasma LPS level, and ZO1 expression were significantly correlated with increased GLP-2 level. The association between bacterial endotoxemia from the gut origin and T2D/obesity has been routinely established by other studies. All the above-mentioned data for berberine is in line with the well-established role played by the gut microbiota in diabetes pathology. Any condition including sleep deprivation that alter the structure of the gut microbiota is thus associated with the development of inflammation in adipose tissues and insulin resistance in animal studies [101]. Accordingly, both obesity and glucose tolerance could be modulated by targeting the gut microbiota [102]. The high blood glucose level associated with obesity in elderly people was also shown to be linked to changes in the gut microbiota [103]. The differential structure and composition of the gut microbiota in normal and T2D diabetes patients observed in many studies [104-106] also appear to be the therapeutic target for berberine.
re
3.3. Gut inflammation and microbiota
Jo
ur
na
lP
Berberine is among the most potent natural products which ameliorate inflammatory bowel disease and associated disorders [36]. Some the key findings on the role of the gut microbiota modulation for its anti-inflammatory properties in the gut is summarised in Table 3 [62,107-109]. Berberine also ameliorate mucosal barrier alteration and dysfunction under diabetic and other pathological conditions. Gong et al. [110] have shown that diabetic rats are subjected to proinflammatory intestinal changes, altered gut-derived hormones, and 2.77-fold increase in intestinal permeability which were all reversed by berberine treatment. This effect was also associated with the known effect of berberine as anti-inflammatory agent via the TLR4/MyD88/NF-κB signalling pathways in intestinal tissue [110]. By activating the AMPK activity thereby suppressing IFN-γ- and Il-17A-producing lamina propria CD4+ T cells both in vitro and in vivo, berberine can suppress chronic inflammation including under IBD condition [111]. Berberine can modulate the transcription factor nuclear factor erythroid 2-related factor 2 (Nrf2) signalling both in Caco-2 cells and rat model of colitis [112] as shown for many other antiinflammatory natural products [113]. Intestinal barrier function in nonalcoholic fat liver disease (NAFLD) in rats maintained under high-fat diet could also be reversed by berberine along with improvement on anti-inflammatory (LPS and cytokines) and lipid (cholesterol) dysregulation markers [114]. Table 3. Inhibition of gut inflammation by berberine via modulation of the gut microbiota. Bioassay model Diarrhoea from irritable bowel syndrome patients transplanted to rats
Dosage 200 mg/kg, p.o. weeks
for 2
Key finding Alter the level of Faecalibacterium, faecal formate, acetate, and propionate by modulating the gut microbiome composition; decrease
References Jia et al. [107]
DSS-induced colitis in mice
40 mg/kg BBR for 10 days
Zhang et al. [62]
ro of
136.5 mg/kg or metformin at 113.75 mg/kg i.g for 11 weeks
Cui et al. [108]
na
Sequencing on 253 faecal samples from consecutive ITP patients and healthy controls.
lP
re
-p
db/db mice
Firmicutes-to-Bacteroidetes ratio at the phylum level; decrease at the genus level Bacteroides, Faecalibacterium, Ruminococcus, Gemmiger, Roseburia, Clostridium XI, and Lachnospiraceae_incertae_sedis. Reduce serum LPS levels; increase SCFA content in faeces; modulate the ratio of Firmicutes-to-Bacteroidetes; increase the proportions of Butyricimonas, Lactobacillus, Coprococcus, Ruminococcus, and Akkermansia; reduce the proportions of Prevotella and Proteus. Increase the relative abundance of Eubacterium while reducing Desulfovibrio in the disease model; Bacteroides abundance even higher than the level in healthy animals; effect on Treg/Th17 balance was ameliorated after the depletion (by combination of ciprofloxacin and metronidazole treatment) of gut microbiota. Improve the microbial dysbiosis of corticosteroid-resistant ITP patients; reverse the effect of L. bacterium colonization on gut microbiota structure.
Wang et al. [109]
ur
Abbreviations: ITP, Thrombocytopenia; Treg, regulatory T cells.
Jo
The anti-inflammatory effect and amelioration of ulcerative colitis in rats by berberine was shown to be associated with modulation of the gut microbiota [108]. In this DSS-induced colitis model in mice, berberine treatment could recover body weight loss and decreased loss of colon length, mucosal necrosis and the associated inflammation. They also noted the ratio of CD4+IL17A+(Th17) cells in spleen lymphocytes were increased while the proportion of CD4+CD25+Foxp3+(Treg or regulatory T cells) cells in spleen lymphocytes were decreased by berberine treated animals with colitis. Hence, berberine treatment could improve the Treg/Th17 balance in the DSS-induced colitis model. Even though the most abundant phyla in all animal groups were Bacteroidetes, Firmicutes, and Proteobacteria, those treated with berberine have Proteobacteria, Streptococcaceae, Enterococcaceae, and Erysipelotrichale as predominant intestinal flora. While the relative abundance of various groups could be modified by berberine (Table 3), the effect of berberine on the Treg/Th17 balance was lost after the depletion (by combination of ciprofloxacin and metronidazole treatment) of the gut microbiota. Hence, the antiinflammatory effect of berberine in this colitis model was induced through modulation of the
na
lP
re
-p
ro of
microbiota. Based on meta-analysis of twenty-three randomized controlled trials with a total of 1763 patients of active ulcerative colitis, probiotics have been shown to have additional benefit in inducing remission [115]. This is consistent with experimental data in animal studies where probiotics ameliorate colitis by increasing Treg [116]. In this direction, the role of SCFAs, as microbial product to regulate the size and function of the colonic Treg pool and protect against colitis in mice have been established [117]. When the faecal microbiota from diarrhoea-predominant irritable bowel syndrome patients were transplanted to rats, it was shown to induce significant Kupffer cell hyperplasia, hepatic sinusoid hypertrophy, and elevated levels of hepatic TNF-α and interferon-γ and a decrease in the synthesis of ALB [107]. Under this condition, berberine could partially reverse the Kupffer cell hyperplasia, Faecalibacterium, faecal formate, acetate, and propionate levels by modulating the gut microbiome composition. It was also shown that treatment with berberine can significantly change the structure and profile of the faecal microbiome of the disease group (Table 3). As discussed for obesity and diabetes conditions, Rajilić-Stojanović et al. [118] have shown that the microbiota of IBS patients when compared with controls, had a “2-fold increased ratio of the Firmicutes to Bacteroidetes resulting from an approximately 1.5-fold increase in numbers of Dorea, Ruminococcus, and Clostridium spp; a 2-fold decrease in the number of Bacteroidetes; a 1.5-fold decrease in numbers of Bifidobacterium and Faecalibacterium spp; and, when present, a 4-fold lower average number of methanogens”. While the degree of changes may depend on the severity of the diseases and doses of therapeutic agents, the effect of berberine appears to be in line with these observations. Wang et al. [109] have shown that dysbiosis was detected in the gut microbiome of Thrombocytopenia (ITP) patients with Lachnospiraceae bacterium, Clostridium asparagiforme were overrepresented while Bacteroides spp was depleted when compared with healthy controls. In this case, berberine treatment could improve the microbial dysbiosis of corticosteroid-resistant ITP patients (Table 3). Interestingly, berberine but not antibiotics, enhance the response to corticosteroid therapy by reversing the effect of L. bacterium colonization on gut microbiota structure. This of course needs further research to establish how modulation of L. bacterium could lead to the observed effect. In the antidiabetic activity studies using db/db mice, Zhang et al. [62] showed that berberine and metformin could reverse the disease-mediated reduction in the level of occludin and ZO1 tight junction proteins along with increased SCFA content in faeces and/or reversal of the altered microbiota composition (Table 3). 3.4. Other organoprotective effects
Jo
ur
Given the diverse pharmacological effects of berberine through multiple mechanisms including general anti-inflammatory and antioxidants properties, its organoprotective effect is not surprising. By regulating autophagic flux, berberine can induce hepatoprotective effect under high level of cholesterol [66]. Hence, it induces neuroprotective effects in cellular models such as SH-SY5Y and PC12 cells [119,120], in animal models [121,122] and under clinical conditions [123]. The hepatoprotective [124,125], cardioprotective including in humans [126-128] and nephroprotective [129,130] effects, among others, of berberine have been well-established. On these bases and the organoprtective effects under obesity, hyperepidemic and diabetes discussed in the preceding sections, it is interesting to see the link between its organoprotective and modulatory effects in the gut microbiota. Guan et al. [131] have studied the role played by the colon microbiota in the ameliorative effect of berberine on the bleomycin-induced pulmonary fibrosis (PF) in mice. While the mechanisms involved activation of PPAR-γ in lung tissues, they have shown that it was a result of hepatocyte growth factor (HGF) expression in colonic fibroblasts. In this connection, the LPS-induced hepatocyte proliferation via stimulation of HGF has been shown to be suggested as the link between the gut microbiota and liver regeneration [132]. In the gut of liver cirrhosis patients, potentially pathogenic bacteria including the Enterobacteriaceae and Streptococcaceae have been shown to be predominant while the beneficial
bacteria such as Lachnospiraceae exit at lower level [133]. Agents like berberine with a profound effect on the structure of the gut microbiota in health and diseases are thus likely to modulate diseases through such mechanisms. Evidence for the direct link was further provided by the study of Quin et al. [134] which showed that berberine could ameliorate the diethylnitrosamine-induced hepatotoxicity and intestinal damage induced by penicillin or DSS. They have also used faecal microbiota transplantation experiment to demonstrate that the observed beneficial effect of berberine was mediated by homeostatic alteration in the gut microbiota. These data are also consistent with those by Jia et al. [135] which revealed that berberine can alleviate some of the inflammatory damage in germfree rats subjected to faecal microbiota from IBS patients. Other effect of berberine linked to the gut microbiota is related to periodontal bone loss [136]. 3.5. Cancer
Jo
ur
na
lP
re
-p
ro of
Noting the high inter-individual variability in the mice gut microbial composition, Wang et al. [137] studied colorectal cancer development in high-fat obese Apc min/+ mice. As with other experiments discussed in the previous sections, the predominant gut microbiota of wild type mice taxa at the phylum level were Firmicutes (55.7%) and Bacteroidetes (42.28%); and on the lower scale, Proteobacteria (1.69%) and Verrucomicrobia (0.11%). The individual variation in these groups could be up to 55% (Bacteroidetes and Firmicutes) in the wild type mice, while the level of Verrucomicrobia increases (wild type and Apc min/+ mice) by high-fat diet, treatment with berberine appear to ameliorate both the structural changes in microbiota and colorectal cancer development. The association between the effect of berberine on colorectal cancer and microbiota regulation was also investigated by Gao et al. [138]. Their study characterized the faecal microbiota, also known as fungal signature, in 131 subjects, comprising polyp and colorectal cancer (CRC) patients. They reported a distinct fungal dysbiosis and an alteration in the fungal network in polyp and CRC pathogenesis. Whether this pattern could be reversed by natural products such as berberine remains to be investigated. The study by Yu et al. [139] employed a potent carcinogen, 1,2-dimethylhydrazine (DMH) or Fusobacterium nucleatum in mice in the presence or absence of berberine. Treatment with F. nucleatum, for example, could increase the level of opportunistic pathogens such as Tenericutes and Verrucomicrobia both in in wild-type and in mice treated with DMH. Berberine was able to ameliorate this bacterial compositional change along with modulation of inflammatory markers: IL-21/22/31, CD40L and the expression of p-STAT3, p-STAT5 and p-ERK1/2, when compared with mice fed with F. nucleatum alone. The levels of opportunistic pathogens, such as Fusobacterium, Streptococcus and Enterococcus spp. gradually increased during the colorectal adenoma-carcinoma sequence in human faecal and mucosal samples. Readers should note that berberine is by far one of the best studied natural products for direct toxicity to cancer cells such as breast cancer [140], colorectal [141], lung [142], hepatocarcinoma [143], leukaemia [144], etc. By interfering signalling pathways such as the AMPK [145], PI3K/AKT [146,147], miRNA [148,149], and prostaglandin [150], berberine has been shown to suppress cancer metastasis. As an adjuvant or combination therapy, berberine has also been shown to enhance the activity of anticancer drugs such as tamoxifen [151], vincristine [152], cisplatin [153], etc. On these bases and the observed effect of berberine on the gut microbiota, berberine is an example of a natural products that acts through polypharmacology principles. General Summary and Conclusion Berberine is a multifunctional natural product with diverse therapeutic applications. As a potent inhibitor of enzymes such as acetylcholinesterase and its ability to alter the amyloid β-induced pathological changes, its therapeutic potential in neurodegenerative diseases such as Alzheimer’s disease has been advocated [4]. Berberine also possesses antioxidant and anti-inflammatory effects in vivo and its plethora of pharmacological effects as organoprotective agent could be linked to such
lP
re
-p
ro of
properties. The therapeutic potential of berberine is thus through acting on multiple targets of the polypharmacology principle that has been shown for many natural products [22]. Evidences presented in this paper now appear to also show that the effect of berberine is linked to the diverse effects of the gut microbiota in health and disease as depicted in Figure 2.
Jo
ur
na
Figure 2. Modulation of the gut microbiota by berberine in health and disease. The polypharmacology of berberine is associated with the diverse effect of the gut microbiota in health and disease. Berberine has a poor bioavailability and its metabolism and pharmacokinetics are related to the activity of the microbiota. Under normal conditions, the structure and composition of the gut microbiota, partly through increased production of SCFAs, promote health. The reduced level of infection and LPS means low level of inflammation both in the gut and in the circulation which has also implication to improved lipid metabolism and insulin sensitivity. Under pathological conditions, the gut microbiota composition is in favour of pathogenic bacteria proliferation and the resulting gut inflammation with compromised intestinal barrier allow high level of systemic LPS. Altered lipid metabolism and insulin sensitivity are associated with such changes leading to the development of diseases such as hyperlipidaemia-associated cardiovascular diseases, diabetes, neurodegenerative diseases and organ disfunction associated with inflammation and oxidative stress (e.g., liver, kidney, and pulmonary dysfunctions). While berberine has multiple effects through enzyme/receptor and cell signalling mechanisms, a growing evidence now also suggest that it acts through modulation of the gut microbiota structure and composition.
The evidences on the modulation of microbiota by berberine showed a great deal of variability to the extent of changes both in quantitative and qualitative manor. While some evidences show, alteration in F/B ratio, some studies show no effect on this ratio. Although the general trend is that
berberine reverses the suppressed level of SCFAs under pathological conditions, there is also data variability related to which individual SCFA is more affected by berberine. Most of these data variations are also attributed to the inter-individual variations in the composition of the gut microbiota. The effect of berberine on the gut microbiota appears to be similar with the general pharmacology associated with the therapeutic application of probiotics, dietary fibres and other drugs such as metformin. With the call for more scientific research on the above-mentioned data variations, the polypharmacology of berberine is in part explained by its role in modulation of the gut microbiota. Conflicts of Interest: The authors declare no conflict of interest.
Funding: This work did not receive any financial support from either internal or external sources.
References
6. 7. 8.
9.
10.
11.
ro of
Jo
12.
-p
5.
re
4.
lP
3.
na
2.
D. Potdar, R.R. Hirwani, S. Dhulap, Phyto-chemical and pharmacological applications of Berberis aristate, Fitoterapia, 83 (5) (2012) 817-830. A. Singh, S. Duggal, N. Kaur, J. Singh, Berberine: Alkaloid with wide spectrum of pharmacological activities, J Nat Prod 3 (2010) 64-75. S. Habtemariam, The hidden treasure in Europe’s garden plants: Case examples; Berberis darwinni and Bergenia cordifolia, Medicinal & Aromatic Plants 2013, 2, 4. S. Habtemariam, The therapeutic potential of Berberis darwinii stem-bark: quantification of berberine and in vitro evidence for Alzheimer’s disease therapy, Nat. Prod. Commun. 6 (8) (2011) 1089–1090. A. Singh, V. Bajpai, M. Srivastava, K.R. Arya, B. Kumar, Rapid screening and distribution of bioactive compounds in different parts of Berberis petiolaris using direct analysis in real time mass spectrometry, J Pharm Anal 5 (5) (2015) 332-335. R. Suau, R. Rico, J.M. López-Romero, F. Nájera, A. Cuevas, Isoquinoline alkaloids from Berberis Vulgaris subsp. Australis Phytochemistry 49 (8) (1998) 2545-2549. ACS. Berberine. https://www.acs.org/content/acs/en/molecule-of-theweek/archive/b/berberine.html (Accessed, 6 January 2020) D.G. Kim, J.W. Choi, I.J. Jo, M.J. Kim, H.S. Lee, S.H. Hong, et al., Berberine ameliorates lipopolysaccharide-induced inflammatory responses in mouse inner medullary collecting duct-3 cells by downregulation of NF-κB pathway, Mol Med Rep (2019) doi: 10.3892/mmr.2019.10823. M. Takahara, A. Takaki, S. Hiraoka, T. Adachi, Y. Shimomura, H. Matsushita, et al., Berberine improved experimental chronic colitis by regulating interferon-γ- and IL-17A-producing lamina propria CD4+ T cells through AMPK activation, Sci Rep 9(1) (2019) 11934. C. Gong, X. Hu, Y. Xu, J. Yang, L. Zong, C. Wang, et al., Berberine inhibits proliferation and migration of colorectal cancer cells by downregulation of GRP78, Anticancer Drugs (2019) doi: 10.1097/CAD.0000000000000835. F. Jin, T. Xie, X. Huang, X. Zhao, Berberine inhibits angiogenesis in glioblastoma xenografts by targeting the VEGFR2/ERK pathway, Pharm Biol 56 (1) (2018) 665-671. Y. Wang, S. Zhang, Berberine suppresses growth and metastasis of endometrial cancer cells via miR-101/COX-2, Biomed Pharmacother 103 (2018) 1287-1293. Y. Yu, L. Liu, X. Wang, X. Liu, X. Liu, L. Xie, et al., Modulation of glucagon-like peptide-1 release by berberine: in vivo and in vitro studies, Biochem Pharmacol, 79 (7) (2010) 1000-1006. Y. Zhang, X. Li, D. Zou W. Liu, J. Yang, N. Zhu, et al., Treatment of type 2 diabetes and dyslipidemia with the natural plant alkaloid berberine, J Clin Endocrinol Metab 93 (7) (2008) 25592565. H. Zhang, J. Wei, R. Xue J.D. Wu, W. Zhao, Z.Z. Wang, et al., Berberine lowers blood glucose in type 2 diabetes mellitus patients through increasing insulin receptor expression, Metabolism 59 (2010) 285–292.
ur
1.
13. 14.
15.
Jo
ur
na
lP
re
-p
ro of
16. W.S. Kim, Y.S. Lee, S.H. Cha, H.W. Jeong, S.S. Choe, M.R. Lee, et al., Berberine improves lipid dysregulation in obesity by controlling central and peripheral AMPK activity, Am J Physiol Endocrinol Metab 296 (4) (2009) E812-E819. 17. G. Derosa, P. Maffioli, A.F. Cicero, Berberine on metabolic and cardiovascular risk factors: an analysis from preclinical evidences to clinical trials, Expert Opin Biol Th 12 (2012) 1113–1124. 18. Y. Yu, M. Zhang, Y. Hu, Y. Zhao, F. Teng, X. Lv, et al., Increased bioavailable berberine protects against myocardial ischemia reperfusion injury through attenuation of NFκB and JNK signaling pathways, Int Heart J 59 (6) (2018) 1378-1388. 19. K. Wang, Q. Chen, N. Wu, Y. Li, R. Zhang, J. Wang, et al., Berberine Ameliorates Spatial Learning Memory Impairment and Modulates Cholinergic Anti-Inflammatory Pathway in Diabetic Rats. Front Pharmacol 10 (2019) 1003. 20. S. Ghotbi-Ravandi, M. Shabani, H. Bashiri, M. Saeedi Goraghani, M. Khodamoradi, M. Nozari, Ameliorating effects of berberine on MK-801-induced cognitive and motor impairments in a neonatal rat model of schizophrenia, Neurosci Lett 706 (2019) 151-157. 21. S. Sadraie, Z. Kiasalari, M. Razavian, S. Azimi, L. Sedighnejad, S. Afshin-Majd, et al., Berberine ameliorates lipopolysaccharide-induced learning and memory deficit in the rat: insights into underlying molecular mechanisms, Metab Brain Dis 2019 34 (1) 245-255. 22. S. Habtemariam, Going back to the good old days: The merit of crude plant drug mixtures in the 21st century, Int J Complement Alt Med 6 (2) (2017) 00182 23. W. Chen, Y.Q. Miao, D.J. Fan, S.S. Yang, X. Lin, L.K. Meng, et al., Bioavailability study of berberine and the enhancing effects of TPGS on intestinal absorption in rats, AAPS PharmSciTech 12 (2011) 705–711. 24. G.Y. Pan, G.J. Wang, X.D. Liu, J.P. Fawcett, Y.Y. Xie, The involvement of P‐glycoprotein in berberine absorption, Pharmacol Toxicol 91 (2002) 193–197. 25. Y.T. Liu, H.P. Hao, H.G. Xie, L. Lai, Q. Wang, C.X. Liu, et al., Extensive intestinal first-pass elimination and predominant hepatic distribution of berberine explain its low plasma levels in rats. Drug Metab Dispos 38 (2010) 1779–1784. 26. S.H. Gu, B. Cao, R.B. Sun, Y.Q. Tang, J.L. Paletta, X.L. Wu, et al., A metabolomic and pharmacokinetic study on the mechanism underlying the lipid-lowering effect of orally administered berberine, Molecular Biosystems 11 (2) (2015) 463-474. 27. W. Hua, L. Ding, Y. Chen, B. Gong, J. He, G. Xu, Determination of berberine in human plasma by liquid chromatography–electrospray ionization–mass spectrometry, J Pharmaceut Biomed 44 (2007) 931–937. 28. X.S. Tan, J.Y. Ma, R. Feng, C. Ma, W.J. Chen, Y.P. Sun, et al., Tissue distribution of berberine and its metabolites after oral administration in rats. PloS One 8 (2013) e77969. 29. R. Feng, Z.X. Zhao, S.R. Ma, F. Guo, Y. Wang, J.D. Jiang, Gut Microbiota-regulated pharmacokinetics of berberine and active Metabolites in Beagle dogs after oral administration, Front Pharmacol 9 (2018) 214. 30. H.W. Xin, X.C. Wu, Q. Li, A.R. Yu, M.Y. Zhong, Y.Y. Liu, The effects of berberine on the pharmacokinetics of cyclosporin A in healthy volunteers, Methods Find Exp Clin Pharmacol 28 (1) (2006) 25-29. 31. Y.F. Lyu, Y.F. Zhang, M.B. Yang, L. Lin, X. Yang, S.C.K. Cheung, et al., Pharmacokinetic interactions between metformin and berberine in rats: Role of oral administration sequences and microbiota, Life Sciences 235 (2019) 116818. 32. Y. Guo, Y.C. Zhang, W.H. Huang, F.P. Selwyn, C.D. Klaassen, Dose-response effect of berberine on bile acid profile and gut microbiota in mice, BMC Complement Altern Med 16 (1) (2016) 394. 33. R.N. Alolga, Y. Fan, Z. Chen, L.W. Liu, Y.J. Zhao, J. Li, et al., Significant pharmacokinetic differences of berberine are attributable to variations in gut microbiota between Africans and Chinese, Sci Rep 6 (2016) 27671. 34. R. Feng, J.W. Shou, Z.X. Zhao, C.Y. He, C. Ma, M. Huang, et al., Transforming berberine into its intestine-absorbable form by the gut microbiota, Sci Rep 5 (2015) 12155.
Jo
ur
na
lP
re
-p
ro of
35. Y. Wang, J.W. Shou, X.Y. Li, Z.X. Zhao, J. Fu, C.Y. He, et al., Berberine-induced bioactive metabolites of the gut microbiota improve energy metabolism, Metab Clin Exp 70 (2017) 72-84. 36. S. Habtemariam, Berberine and inflammatory bowel disease: A concise review, Pharmacol Res 113 (Pt A) (2016) 592-599. 37. M.L. Freile, F. Giannini, G. Pucci, A. Sturniolo, L. Rodero, O. Pucci, et al., Antimicrobial activity of aqueous extracts and of berberine isolated from Berberis heterophylla, Fitoterapia 74 (7–8) (2003) 702– 705. 38. K. Karaosmanoglu, N.A. Sayar, I.A. Kurnaz, B.S. Akbulut, Assessment of berberine as a multitarget antimicrobial: a multi-omics study for drug discovery and repositioning, OMICS 18 (1) (2014) 42–53. 39. Z. Lv, G. Peng W. Liu, H. Xu, J. Su, Berberine blocks the relapse of Clostridium difficile infection in C57BL/6 mice after standard vancomycin treatment, Antimicrob Agents Chemother 59 (7) (2015) 3726-3735. 40. C. Chen, C. Tao, Z. Liu, M. Lu, Q. Pan, L. Zheng, et al., Randomized clinical trial of berberine hydrochloride in patients with diarrhea-predominant irritable bowel syndrome, Phytother Res 29 (11) (2015) 1822–1827. 41. M. Cernakova, D. Kostalova, Antimicrobial activity of berberine - a constituent of Mahonia aquifolium, Folia Microbiol (Praha) 47 (4) (2002) 375–378. 42. S.H. Chae, I.H. Jeong, D.H. Choi, J.W. Oh, Y.J. Ahn, Growth-inhibiting effects of Coptis japonica rootderived isoquinoline alkaloids on human intestinal bacteria. J Agric Food Chem 47 (3) (1999) 934– 938. 43. V.T. Do, B.G. Baird, D.R. Kockler, Probiotics for maintaining remission of ulcerative colitis in adults. Ann Pharmacother 44 (3) (2010) 565–571. 44. D. Haller, J.M. Antoine, S. Bengmark, P. Enck, G.T. Rijkers, I. Lenoir-Wijnkoop, Guidance for substantiating the evidence for beneficial effects of probiotics: probiotics in chronic inflammatory bowel disease and the functional disorder irritable bowel syndrome, J Nutr 140 (3) (2010) 690S– 697S. 45. A.J. Riquelme, M.A. Calvo, M.A. Guzmán, M.S. Depix, P. García, C.M. Pérez, et al., Saccharomyces cerevisiae fungemia after Saccharomyces boulardii treatment in immunocompromised patients, J Clin Gastroenterol 36 (1) (2003) 41–43. 46. W. Sandborn, R. McLeod, D. Jewell, Pharmacotherapy for inducing and maintaining remission in pouchitis, Cochrane Database Syst Rev 2 (2002) CD001176. 47. S.J. Yue, J. Liu, W.X. Wang, A.T. Wang, X.Y. Yang, H.S. Guan, et al., Berberine treatment-emergent mild diarrhea associated with gut microbiota dysbiosis, Biomed Pharmacother 116 (2019) 109002. 48. H.Y. Zhang, X.S. Piao, Q. Zhang, P. Li, J.Q. Yi, J.D. Liu, et al., The effects of Forsythia suspensa extract and berberine on growth performance, immunity, antioxidant activities, and intestinal microbiota in broilers under high stocking density, Poultry Science 92 (8) (2013) 1981-1988. 49. R.E. Ley, M. Hamady, C. Lozupone, P.J. Turnbaugh, R.R. Ramey, J.S. Bircher, et al., Evolution of mammals and their gut microbes, Science 320 (5883) (2008) 1647-1651. 50. Y. Yang, F. Liu, R. Lu, J. Jia, Berberine Inhibits Adipogenesis in Porcine Adipocytes via AMPActivated Protein Kinase-Dependent and -Independent Mechanisms, Lipids 54 (11-12) (2019) 667678. 51. Y.Y. Wu, X.M. Huang, J. Liu, Y. Cha, Z.P. Chen, F. Wang, et al., Functional study of the upregulation of miRNA-27a and miRNA-27b in 3T3-L1 cells in response to berberine, Mol Med Rep 14 (3) (2016) 2725-31. 52. C. Wang, Y. Wang, S.R. Ma, Z.Y. Zuo, Y.B. Wu, W.J. Kong, et al., Berberine inhibits adipocyte differentiation, proliferation and adiposity through down-regulating galectin-3, Sci.Rep 9 (1) (2019) 13415. 53. J. Zhang H. Tang R. Deng N. Wang Y. Zhang Y. Wang et al., Berberine suppresses adipocyte differentiation via decreasing CREB transcriptional activity, PLoS One 10 (4) (2015) e0125667.
Jo
ur
na
lP
re
-p
ro of
54. Z. Zhang, H. Zhang, B. Li, X. Meng, J. Wang, Y. Zhang, et al., Berberine activates thermogenesis in white and brown adipose tissue, Nat Commun 5 (2014) 5493. 55. Z. Li, J.D. Jiang, W.J. Kong, Berberine up-regulates hepatic low-density lipoprotein receptor through ras-independent but AMP-activated protein kinase-dependent Raf-1 activation, Biol Pharm Bull 37 (2014) 1766–1775. 56. H.D. Sun, Q. Liu, H. Hu, Y.S. Jiang, W.T. Shao, Q.H. Wang, et al., Berberine ameliorates blockade of autophagic flux in the liver by regulating cholesterol metabolism and inhibiting COX2prostaglandin synthesis, Cell Death Dis 9 (2018) 824 57. Y. Hu, G.E. Davies, Berberine inhibits adipogenesis in high-fat diet-induced obesity mice, Fitoterapia 81 (2010) 358–366. 58. Y. Hu, E.A. Ehli, J. Kittelsrud, P.J. Ronan, K. Munger, T. Downey, et al., Lipid-lowering effect of berberine in human subjects and rats, Phytomedicine 19 (10) (2012) 861-867. 59. W.S. Kim, Y.S. Lee, S.H. Cha, H.W. Jeong, S.S. Choe, M.R. Lee, et al., Berberine improves lipid dysregulation in obesity by controlling central and peripheral AMPK activity, Am J Physiol Endocrinol Metab 296 (4) (2009) E812-9. 60. W. Kong, J. Wei, P. Abidi, M. Lin, S. Inaba, C. Li, et al., Berberine is a novel cholesterol-lowering drug working through a unique mechanism distinct from statins, Nat Med 10 (2004) 1344–1351. 61. H.H. Guo, C. Ma, W.S. Zheng, Y. Luo, C. Li, X.L. Li, et al., Dual-Stimuli-Responsive Gut MicrobiotaTargeting Berberine-CS/PT-NPs Improved Metabolic Status in Obese Hamsters, Adv. Funct. Mater. 29 (14) (2019) doi: 10.1002/adfm.201808197 62. W. Zhang, J.H. Xu, T. Yu, Q.K. Chen, Effects of berberine and metformin on intestinal inflammation and gut microbiome composition in db/db mice, Biomed Pharmacother 118 (2019) 109131. 63. L. Zhu, D.Y. Zhang, H. Zhu, J.M. Zhu, S.G. Weng, L. Dong, et al., Berberine treatment increases Akkermansia in the gut and improves high-fat diet-induced atherosclerosis in Apoe(-/-) mice, Atherosclerosis 268 (2018) 117-126. 64. Y.F. Shi, J.X. Hu, J. Geng, T.T. Hu, B.J. Wang, W.T. Yan, et al., Berberine treatment reduces atherosclerosis by mediating gut microbiota in apoE-/- mice, Biomed Pharmacother 107 (2018) 1556-1563. 65. H. Wang, L.N. Guan, J. Li, M.D. Lai, X.D. Wen, The effects of berberine on the gut microbiota in Apc (min/+) mice fed with a high fat diet, Molecules 23 (9) (2018) pii: E2298. 66. Y. Sun, C. Jin, X. Zhang, W. Jia, J. Le, J. Ye, Restoration of GLP-1 secretion by Berberine is associated with protection of colon enterocytes from mitochondrial overheating in diet-induced obese mice, Nutr Diabetes 8 (1) (2018) 53. 67. J.H. Xu, X.Z. Liu, W. Pan, D.J. Zou, Berberine protects against diet-induced obesity through regulating metabolic endotoxemia and gut hormone levels, Mol Med Rep 15 (5) (2017) 2765-2787. 68. Y. Wang, Q. Tong, J.W. Shou, Z.X. Zhao, X.Y. Li, X.F. Zhang, et al., Gut microbiota-mediated personalized treatment of hyperlipidemia using berberine, Theranostics 7 (9) (2017) 2443-2451. 69. R.B. Sun, N. Yang, B. Kong, B. Cao, D. Feng, X.Y. Yu, et al., Orally administered berberine modulates hepatic lipid metabolism by altering microbial bile acid metabolism and the intestinal FXR signaling pathway, Mol Pharmacol 9 (2) (2017) 110-122. 70. Y. Cao, Q. Pan, W. Cai, F. Shen, G.Y. Chen, L.M. Xu, et al., Modulation of gut microbiota by berberine improves steatohepatitis in high-fat diet-fed BALB/C mice, Arch Iran Med 19 (3) (2016) 197-203. 71. M. Li, X.B. Shu, H.C. Xu, C.L. Zhang, L.L. Yang, L. Zhang, et al., Integrative analysis of metabolome and gut microbiota in diet-induced hyperlipidemic rats treated with berberine compounds, J Trans Med 14 (1) (2016) 237. 72. H.L. Sun, N.J. Wang, Z. Cang, C.X. Zhu, L. Zhao, X.M. Nie, et al., Modulation of microbiota-gutbain axis by berberine resulting in improved metabolic status in high-fat diet-fed rats, Obesity Facts 9 (6) (2016) 365-378.
Jo
ur
na
lP
re
-p
ro of
73. X. Zhang, Y.F. Zhao, J. Xu, Z.S. Xue, M.H. Zhang, X.Y. Pang, et al., Modulation of gut microbiota by berberine and metformin during the treatment of high-fat diet-induced obesity in rats, Sci Rep 5 (2015) 14405. 74. X. Zhang, Y.F. Zhao, M.H. Zhang, X.Y. Pang, J. Xu, C.Y. Kang, et al., Structural changes of gut microbiota during berberine-mediated prevention of obesity and insulin resistance in high-fat diet-fed rats, Plos One 7 (8) (2012) e42529. 75. R.E. Ley, F. Bäckhed, P. Turnbaugh, C.A. Lozupone, R.D. Knight, J.I. Gordon, Obesity alters gut microbial ecology, Proc Natl Acad Sci USA 102 (2005) 11070–11075. 76. M. Begley, C. Hill C.G. Gahan, Bile salt hydrolase activity in probiotics, Appl Environ Microbiol. 72 (3) (2006) 1729-1738. 77. I. De Smet, L. Van Hoorde, M. Vande Woestyne, H. Christiaens, W. Verstraete, Significance of bile salt hydrolytic activities of lactobacilli, J Appl Bacteriol 79 (3) (1995) 292-301. 78. F. Li, C. Jiang, KW. Krausz, Y. Li, I. Albert, H. Hao, et al., Microbiome remodelling leads to inhibition of intestinal farnesoid X receptor signalling and decreased obesity, Nat Commun 4 (2013) 2384. 79. J. Lan, Y. Zhao, F. Dong, Z. Yan, W. Zheng, J. Fan, et al., Meta-analysis of the effect and safety of berberine in the treatment of type 2 diabetes mellitus, hyperlipemia and hypertension, J Ethnopharmacol 161 (2015) 69-81 80. J. Yin, H. Xing, J. Ye, Efficacy of berberine in patients with type 2 diabetes mellitus, Metabolism 57 (2008) 712–717. 81. Y. Zhang, X. Li, D. Zou, W. Liu, J. Yang, N. Zhu, et al., Treatment of type 2 diabetes and dyslipidemia with the natural plant alkaloid berberine, J Clin Endocrinol Metab 93 (7) (2008) 255965. 82. H. Zhang, J. Wei, R. Xue, J-D. Wu, W. Zhao, Z.Z. Wang, et al., Berberine lowers blood glucose in type 2 diabetes mellitus patients through increasing insulin receptor expression. Metabolism 59 (2010) 285–292. 83. L.Z. Liu, S.C. Cheung, L.L. Lan, S.K. Ho, H.X. Xu, J.C. Chan, et al., Berberine modulates insulin signaling transduction in insulin-resistant cells, Mol Cell Endocrinol 317 (2010) 148–153. 84. B-S. Ko, S.B. Choi, S.K. Park, J.S. Jang, Y.E. Kim, Park, S. Insulin sensitizing and insulinotropic action of berberine from Cortidis rhizome, Biol Pharm Bull 28 (2005) 1431–1437. 85. H. Dong, Y. Zhao, L. Zhao, F. Lu, The effects of berberine on blood lipids: a systemic review and meta-analysis of randomized controlled trials, Planta Med 79 (2013) 437-446. 86. S.S. Lu, Y.L. Yu, H.J. Zhu, X.D. Liu, L. Liu, Y.W. Liu, et al. Berberine promotes glucagon-like peptide-1 (7–36) amide secretion in streptozotocin-induced diabetic rats, J Endocrinol 200 (2009) 159–165. 87. W. Chang, M. Zhang, Z. Meng, Y. Yu, F. Yao, G.M. Hatch, et al., Berberine treatment prevents cardiac dysfunction and remodeling through activation of 5’-adenosine monophosphateactivated protein kinase in type 2 diabetic rats and in palmitate-induced hypertrophic H9c2 cells, Eur J Pharmacol 769 (2015) 55–63. 88. J. Yin, Z. Gao, D. Liu, Z. Liu, J. Ye, Berberine improves glucose metabolism through induction of glycolysis, Am J Physiol Endocrinol Metab 294 (2008) E148–E156. 89. L.F. Ye, S. Liang, C. Guo, X.Z. Yu, J. Zhao, H. Zhang, et al., Inhibition of M1 macrophage activation in adipose tissue by berberine improves insulin resistance, Life Sci 166 (2016) 82-91. 90. X. Xia, J. Yan, Y. Shen, K. Tang, J. Yin, Y. Zhang, et al., Berberine improves glucose metabolism in diabetic rats by inhibition of hepatic gluconeogenesis, PLoS One 6 (2011) e16556. 91. H.J. Pan, Z.F. Li, J. Xie, D. Liu, H.J. Wang, D.G. Yu, et al., Berberine influences blood glucose via modulating the gut microbiome in grass carp, Front Microbiol 10 (2019) 1066.
Jo
ur
na
lP
re
-p
ro of
92. S.J. Yue, J. Liu, A.T. Wang, X.T. Meng, Z.R. Yang, C. Peng, et al., Berberine alleviates insulin resistance by reducing peripheral branched-chain amino acids, Am J Physiol Endocrinol Metab 316 (1) (2019) E73-E85. 93. Y. Tian, J.W. Cai, W. Gui, R.G. Nichols, I. Koo, J.T. Zhang, et al., Berberine directly sffects the gut microbiota to promote intestinal farnesoid X receptor activation, Drug Metab Dispos 47 (2) (2019) 86-93. 94. H.X. Cui, Y.N. Hu, J.W. Li, K. Yuan, Hypoglycemic mechanism of the berberine organic acid salt under the synergistic effect of intestinal flora and oxidative stress, Oxid Med Cell Longev 2018 (2018) 8930374. 95. D. Liu, Y.Y. Zhang, Y.H. Liu, L.Q. Hou, S.Y. Li, H.M. Tian, et al., Berberine modulates gut microbiota and reduces insulin resistance via the TLR4 signaling pathway, Exp Clin Endocrinol Diabets 126 (8) (2018) 513-520. 96. L.L. Chen, W.S. Lu, Y.S. Li, Berberine ameliorates type 2 diabetes via modulation of Bifidobacterium species, tumor necrosis factor-alpha, and lipopolysaccharide, Int. J Clin Exp Med 9 (6) (2016) 9365-9372. 97. C.Y. Shan, J.H. Yang, Y. Kong, X.Y. Wang, M.Y. Zheng, Y.G. Xu, et al., Alteration of the intestinal barrier and GLP2 secretion in Berberine-treated type 2 diabetic rats, J Endocrinol 218 (3) (2013) 255262. 98. H. Lee, G. Ko, Effect of metformin on metabolic improvement and gut microbiota, Appl Environ Microbiol 80 (2014) 5935–5943. 99. Z. Gao, J. Yin, J. Zhang, R.E. Ward, R.J. Martin, M. Lefevre, et al., Butyrate improves insulin sensitivity and increases energy expenditure in mice, Diabetes 5 (2009) 1509–1517. 100. H. Yadav, J.H. Lee, J. Lloyd, P. Walter, S.G. Rane, Beneficial metabolic effects of a probiotic via butyrate-induced GLP-1 hormone secretion, J Biol Chem 288 (2013) 25088–25097. 101. V.A. Poroyko, A. Carreras, A. Khalyfa, A.A. Khalyfa, V. Leone, E. Peris, et al., Chronic sleep disruption alters gut microbiota, induces systemic and adipose tissue inflammation and insulin resistance in mice, Sci Rep 6 (1) (2016) 35405. 102. G.V. Bech-Nielsen, C.H. Hansen, M.R. Hufeldt, D.S. Nielsen, B. Aasted, F.K. Vogensen, et al., Manipulation of the gut microbiota in C57BL/6 mice changes glucose tolerance without affecting weight development and gut mucosal immunity, Res Vet Sci 92 (3) (2012) 501–508, 103. E. Sepp, H. Kolk, K. Lõivukene, M. Mikelsaar, Higher blood glucose level associated with body mass index and gut microbiota in elderly people. Higher blood glucose level associated with body mass index and gut microbiota in elderly people, Microb Ecol Health Dis 25 (2014) 22857. 104. N. Larsen, F.K. Vogensen, F.W. van den Berg, D.S. Nielsen, A.S. Andreasen, B.K. Pedersen, et al., Gut microbiota in human adults with type 2 diabetes differs from non-diabetic adults, PLoS One 5 (2) (2010) e9085. 105. H.K. Pedersen, V. Gudmundsdottir, H.B. Nielsen, T. Hyotylainen, T. Nielsen, B.A. Jensen, et al., Human gut microbes impact host serum metabolome and insulin sensitivity, Nature 535 (7612) (2016) 376–381. 106.X. Wu, C. Ma, L. Han, M. Nawaz, F. Gao, X. Zhang, et al., Molecular characterisation of the faecal microbiota in patients with type II diabetes, Curr Microbiol 61 (1) (2010) 69–78. 107.Q. Jia, L. Zhang, J.D. Zhang, F. Pei, S.W. Zhu, Q.H. Sun, et al., Fecal microbiota of diarrheapredominant irritable bowel syndrome patients causes hepatic inflammation of germ-free rats and berberine reverses it partially, Biomed Res Int 2019 (2019) 4530203. 108. H.T. Cui, Y.Z. Cai, L. Wang, B.T. Jia, J.C. Li, S.W. Zhao, et al., Berberine regulates Treg/Th17 balance to treat ulcerative colitis through modulating the gut microbiota in the colon, Front Pharmacol 9 (2018) 571.
Jo
ur
na
lP
re
-p
ro of
109. Y.N. Wang, X. Liu, Y. He, Q.M. Wang, X.L. Zhu, C.C. Wang, et al., Berberine may correct corticosteroid resistance induced by gut microbiota dysbiosis in immune thrombocytopenia, Blood 132 (Suppl. 1) (2018) 3769-3769. 110. J. Gong, M.L. Hu, Z.Y. Huang, K. Fang, D.K Wang, Q. J. Chen, et al., Berberine attenuates intestinal mucosal barrier dysfunction in type 2 diabetic rats, Front Pharmacol 8 (2017) 42. 111. M. Takahara, A. Takaki, S. Hiraoka, T. Adachi, Y. Shimomura, H. Matsushita, et al., Berberine improved experimental chronic colitis by regulating interferon-γ- and IL-17A-producing lamina propria CD4+ T cells through AMPK activation, Sci Rep 9 (1) (2019) 11934. 112. W. Jing, Y. Safarpour, T. Zhang, P. Guo, G. Chen, X. Wu, et al., Berberine upregulates Pglycoprotein in human Caco-2 cells and in an experimental model of colitis in the rat via activation of Nrf2-dependent mechanisms, J Pharmacol Exp Ther 366 (2) (2018) 332-340 113. S. Habtemariam, The Nrf2/HO-1 axis as targets for flavanones: Neuroprotection by pinocembrin, naringenin and eriodictyol, Oxid Med Cell Longev 2019 (2019) 4724920. 114. D. Li, J. Zheng, Y. Hu, H. Hou, S. Hao, N. Liu, et al., Amelioration of intestinal barrier dysfunction by berberine in the treatment of nonalcoholic fatty liver disease in rats, Pharmacogn Mag 13 (52) (2017) 677-682. 115. J. Shen, Z.X. Zuo, A.P. Mao, Effect of probiotics on inducing remission and maintaining therapy in ulcerative colitis, Crohn's disease, and pouchitis: meta-analysis of randomized controlled trials, Inflamm Bowel Dis 20 (1) (2014) 21-35. 116. H.M. Zhao, X.Y. Huang, Z.Q. Zuo, Q.H. Pan, M.Y. Ao, F. Zhou, et al., Probiotics increase T regulatory cells and reduce severity of experimental colitis in mice, World J Gastroenterol 19 (5) (2013) 742-749. 117. P.M. Smith, M.R. Howitt, N. Panikov, M. Michaud, C.A. Gallini, Y.M. Bohlooly, et al., The microbial metabolites, short-chain fatty acids, regulate colonic Treg cell homeostasis, Science 341 (2013) 569– 573. 118. M. Rajilić-Stojanović, E. Biagi, H.J. Heilig, K. Kajander, RA. Kekkonen, S. Tims, et al., Global and deep molecular analysis of microbiota signatures in fecal samples from patients with irritable bowel syndrome, Gastroenterology 141 (5) (2011) 1792–1801. 119. G.E. Buján, H.A. Serra, S.J. Molina, L.R. Guelman, Prevention of brain damage triggered by alcohol consumption during adolescence: Focus on oxidative stress, Curr Pharm Des (2019) doi: 10.2174/1381612825666191209121735 120. H.R. Sadeghnia, M. Kolangikhah, E. Asadpour, F. Forouzanfar, H. Hosseinzadeh, Berberine protects against glutamate-induced oxidative stress and apoptosis in PC12 and N2a cells, Iran J Basic Med Sci 20 (5) (2017) 594-603. 121. S.N. Maleki, N. Aboutaleb, F. Souri, Berberine confers neuroprotection in coping with focal cerebral ischemia by targeting inflammatory cytokines, J Chem Neuroanat 87 (2018) 54-59. 122. J.S. de Oliveira, F.H. Abdalla, G.L. Dornelles, S.A. Adefegha, T.V. Palma, C. Signor, et al., Berberine protects against memory impairment and anxiogenic-like behavior in rats submitted to sporadic Alzheimer's-like dementia: Involvement of acetylcholinesterase and cell death, Neurotoxicology 57 (2016) 241-250. 123. N.N. Yuan, C.Z. Cai, M.Y. Wu, H.X. Su, M. Li, J.H. Lu, Neuroprotective effects of berberine in animal models of Alzheimer's disease: a systematic review of pre-clinical studies, BMC Complement Altern Med 19 (1) (2019) 109. 124. S. Mehrzadi, I. Fatemi, M. Esmaeilizadeh, H. Ghaznavi, H. Kalantar, M. Goudarzi, Hepatoprotective effect of berberine against methotrexate induced liver toxicity in rats, Biomed. Pharmacother 97 (2018) 233-239. 125. Z. Zhao, Q. Wei, W. Hua, Y. Liu, X. Liu, Y. Zhu, Hepatoprotective effects of berberine on acetaminophen-induced hepatotoxicity in mice, Biomed Pharmacother 103 (2018) 1319-1326. 126. Y. Qing, X. Dong, L. Hongli, L. Yanhui, Berberine promoted myocardial protection of postoperative patients through regulating myocardial autophagy, Biomed Pharmacother 105 (2018) 1050-1053.
Jo
ur
na
lP
re
-p
ro of
127. Y. Yu, M. Zhang, Y. Hu, Y. Zhao, F. Teng, X. Lv, et al., Increased Bioavailable Berberine Protects Against Myocardial Ischemia Reperfusion Injury Through Attenuation of NFκB and JNK Signaling Pathways, Int Heart J 59 (6) (2018) 1378-1388. 128. G.L. Zhao, L.M. Yu, W.L. Gao, W.X. Duan, B. Jiang, X.D. Liu, et al., Berberine protects rat heart from ischemia/reperfusion injury via activating JAK2/STAT3 signaling and attenuating endoplasmic reticulum stress, Acta Pharmacol Sin 37 (3) (2016) 354-367 129. R. Domitrović, O. Cvijanović, E. Pernjak-Pugel, M. Skoda, L. Mikelić, Z. Crnčević-Orlić, Berberine exerts nephroprotective effect against cisplatin-induced kidney damage through inhibition of oxidative/nitrosative stress, inflammation, autophagy and apoptosis, Food Chem Toxicol 62 (2013) 397-406. 130. P. Hasanein, H. Riahi, Preventive use of berberine in inhibition of lead-induced renal injury in rats, Environ Sci Pollut Res Int 25 (5) (2018) 4896-4903. 131.C.G. Guan, S.M. Qiao, Q. Lv, N. Cao, K. Wang, Y. Dai, et al., Orally administered berberine ameliorates bleomycin-induced pulmonary fibrosis in mice through promoting activation of PPARgamma and subsequent expression of HGF in colons, Toxicol Appl Pharmacol 343 (2018) 1-15. 132.H.X. Liu, R. Keane, L. Sheng, Y.J. Wan, Implications of microbiota and bile acid in liver injury and regeneration, J Hepatol 63 (6) (2015) 1502–1510. 133.Y. Chen, F. Yang, H. Lu, B. Wang, Y. Chen, D. Lei, et al., Characterization of fecal microbial communities in patients with liver cirrhosis, Hepatology 54 (2) (2011) 562–572. 134.C.J. Qin, H.L. Zhang, L.H. Zhao, M. Zeng, W.J. Huang, G.B. Fu, et al., Microbiota transplantation reveals beneficial impact of berberine on hepatotoxicity by improving gut homeostasis, Sci ChinaLife Sci 61 (12) (2018) 1537-1544. 135. Q. Jia, L. Zhang, J.D. Zhang, S.W. Zhu, Q.H. Sun, L.P. Duan, Berberine patrtyially revised the effects of IBS-D patients fecal microbhiota induced hepatic inflammation in germ-free rats, Gastroenterology 154 (6) (2018) S1126-S1126. 136. X. Jia, L. Jia, L. Mo, S. Yuan, X. Zheng, J. He, et al., Berberine ameliorates periodontal bone loss by regulating gut microbiota, J Dent Res 98 (1) (2019) 107-116. 137. H. Wang, L. Guan, J. Li, M. Lai, X. Wen, The effects of berberine on the gut microbiota in Apc min/+ mice fed with a high fat diet, Molecules 23 (9) (2018) pii: E2298. 138. R. Gao, C. Kong, H. Li, L. Huang, X. Qu, N. Qin, et al., Dysbiosis signature of mycobiota in colon polyp and colorectal cancer, Eur J Clin Microbiol Infect Dis 36 (12) (2017) 2457-2468. 139. Y.N. Yu, TC. Yu, H.J. Zhao, T.T. Sun, H.M. Chen, H.Y. Chen, et al., Berberine may rescue Fusobacterium nucleatum-induced colorectal tumorigenesis by modulating the tumor microenvironment, Oncotarget 6 (31) (2015) 32013-32026. 140. Y. Sun, W. Wang, Y. Tong, Berberine inhibits proliferative ability of breast cancer Cells by reducing metadherin, Med Sci Monit 25 (2019) 9058-9066. 141. C. Gong, X. Hu, Y. Xu, J. Yang, L. Zong C. Wang et al., Berberine inhibits proliferation and migration of colorectal cancer cells by downregulation of GRP78, Anticancer Drugs (2019) doi: 10.1097/CAD.0000000000000835. 142. Q.Q. Chen, J.M. Shi, Z. Ding, Q. Xia, T.S. Zheng, Y.B. Ren, et al., Berberine induces apoptosis in non-small-cell lung cancer cells by upregulating miR-19a targeting tissue factor, Cancer Manag Res 11 (2019) 9005-9015. 143. F. Li, X. Dong, P. Lin, J. Jiang, Regulation of Akt/FoxO3a/Skp2 axis is critically involved in berberine-induced cell cycle arrest in hepatocellular carcinoma cells, Int J Mol Sci 19 (2) (2018) pii: E327. 144. S. Okubo, T. Uto, A. Goto, H. Tanaka, T. Nishioku, K. Yamada, et al., Berberine induces apoptotic cell death via activation of caspase-3 and -8 in HL-60 human leukemia cells: Nuclear localization and structure-activity relationships, Am J Chin Med 45 (7) (2017) 1497-1511. 145. Q. Hu, L. Li, X. Zou, L. Xu, P. Yi, Berberine attenuated proliferation, invasion and migration by targeting the AMPK/HNF4α/WNT5A pathway in gastric carcinoma, Front Pharmacol 9 (2018) 1150.
Jo
ur
na
lP
re
-p
ro of
146. Y. Kou, L. Li, H. Li, Y. Tan, B. Li, K. Wang, et al., Berberine suppressed epithelial mesenchymal transition through cross-talk regulation of PI3K/AKT and RARα/RARβ in melanoma cells, Biochem Biophys Res Commun 479 (2) (2016) 290-296. 147. L. Li, X. Wang, R. Sharvan, J. Gao, S. Qu, Berberine could inhibit thyroid carcinoma cells by inducing mitochondrial apoptosis, G0/G1 cell cycle arrest and suppressing migration via PI3KAKT and MAPK signaling pathways, Biomed Pharmacother 95 (2017) 1225-1231. 148. C.Y. Lin, P.L. Hsieh, Y.W. Liao, C.Y. Peng, M.Y. Lu, C.H. Yang, et al., Berberine-targeted miR-21 chemosensitizes oral carcinomas stem cells, Oncotarget 8 (46) (2017) 80900-80908. 149. Wang, Y. Zhang, S. Berberine suppresses growth and metastasis of endometrial cancer cells via miR-101/COX-2, Biomed Pharmacother 103 (2018) 1287-1293. 150. X. Liu, Q. Ji, N. Ye, H. Sui, L. Zhou, H. Zhu, et al., Berberine inhibits invasion and metastasis of colorectal cancer cells via COX-2/PGE2 mediated JAK2/STAT3 signaling pathway, PLoS One 10 (5) (2015) e0123478. 151. C. Wen, L. Wu, L. Fu, X. Zhang, H. Zhou, Berberine enhances the anti-tumor activity of tamoxifen in drug-sensitive MCF-7 and drug-resistant MCF-7/TAM cells, Mol Med Rep 14 (3) (2016) 22502256. 152. L. Wang, D. Wei, X. Han, W. Zhang, C. Fan, J. Zhang, et al., The combinational effect of vincristine and berberine on growth inhibition and apoptosis induction in hepatoma cells, J Cell Biochem 115 (4) (2014) 721-730. 153. L. Liu, J. Fan, G. Ai, J. Liu, N. Luo, C. Li, et al., Berberine in combination with cisplatin induces necroptosis and apoptosis in ovarian cancer cells, Biol Res 52 (1) (2019) 37.