Gallbladder motility in obesity, diabetes mellitus and coeliac disease

Digestive and Liver Disease 35 (Suppl. 3) (2003) S12–S16 www.elsevier.com / locate / dld

Gallbladder motility in obesity, diabetes mellitus and coeliac disease M. Fraquelli, M. Pagliarulo, A. Colucci, S. Paggi, D. Conte* Chair of Gastroenterology, University of Milan, Milan, Italy

Abstract We reviewed data on gallbladder motility in obesity, diabetes and coeliac disease. In obesity, a condition characterised by increased risk of gallstone(s), decreased gallbladder motility has heterogeneously been reported as a consequence of the different type of meals used to induce gallbladder contraction, characteristics of the population studied, technique used, and proportion of patients with hyperinsulinaemia. Moreover, recent studies have evaluated the effect of dietary restriction on gallbladder motility in obese patients. A two- to three-fold increase in the risk of cholesterol gallstone(s) has been reported in diabetic patients, mainly in relation to obesity and hypertriglyceridaemia. Furthermore, decreased gallbladder motility has been described and attributed to other factors, including underlying autonomic neuropathy, reduced gallbladder sensitivity to cholecystokinin and / or reduced number of cholecystokinin receptors on the gallbladder wall. Impaired gallbladder motility has been reported also in patients with coeliac disease in relation to reduced secretion of enteric hormones and / or decreased gallbladder sensitivity to them. In particular, untreated coeliacs, when compared to controls, showed low postprandial cholecystokinin and increased fasting somatostatin levels. Interestingly, the correlation between fasting somatostatin levels and gallbladder size has clearly been confirmed in patients affected by somatostatinoma or treated with somatostatin or its analogues. Gallbladder motility can be affected by various clinical conditions, such as obesity, diabetes mellitus and coeliac disease.  2003 Editrice Gastroenterologica Italiana S.r.l. Published by Elsevier Ltd. All rights reserved. Keywords: Coeliac disease; Diabetes mellitus; Gallbladder motility; Obesity; Ultrasound

1. Obesity Obesity is a major risk factor for gallstone disease (GD) [1,2], bile super-saturation, related to the increased synthesis of cholesterol [3], being the main pathogenic factor for gallstone formation. Two other factors also play a relevant role, namely increase in fasting gallbladder (GB) volume and reduction in postprandial (P-P) GB motility. The former has been reported in a number of studies, most of which correlated with body weight, body mass index (BMI) and surface area [4,5], as well as with abdominal fat and impaired glucose tolerance, as in a metabolic syndrome characterised by central adiposity and hyperinsulinaemia [6]. Reduction in P-P GB emptying has been heterogeneously reported (Table 1), probably due to differences in the type of meal used to induce GB contraction, characteristics of the population studied (in terms of BMI, sex, etc.), and technique used to evaluate GB kinetics (i.e., scintigraphy

*Corresponding author. Tel.: 139-02-5503-3418; fax: 139-02-55033644. E-mail address: [email protected] (D. Conte).

or ultrasonography). Conflicting data may also be related to differences in the proportion of obese subjects with hyperinsulinaemia, which can decrease GB sensitivity to cholecystokinin (CCK) with a consequent reduction in GB contraction [7]. Particular interest has been shown in the effect of dietary restriction on obese patients. During rapid weight loss, a significant increase in gallstone disease (GD) has been reported repeatedly, with an overall frequency ranging from 11 to 36% [12]. The underlying pathogenic mechanisms are incompletely understood, but several factors have been considered, including an increase in cholesterol biliary output [13] and / or GB secretion of Table 1 P-P GB motility in obese subjects Author [Ref.]

Patients (n)

Meal type

Technique used

P-P GB a motility

Marzio [8] Acalovschi [9] Stone [10] Vezina [11]

21 44 7 18

Solid Solid Liquid Liquid

US US US Scintigraphy

↓ ND ND ↓

ND, no significant differences; US, ultrasound;↓, decreased. a Versus controls.

1590-8658 / 03 / $30  2003 Editrice Gastroenterologica Italiana S.r.l. Published by Elsevier Ltd. All rights reserved. doi:10.1016 / S1590-8658(03)00087-2

M. Fraquelli et al. / Digestive and Liver Disease 35 ( Suppl. 3) (2003) S12 –S16

mucin and calcium, and a decrease in bile PGE2 and arachidonic acid levels [14,15]. A very low calorie diet also induces GB stasis, possibly as a consequence of reduced GB stimulation [12,16]. In this context, the most important factor is the actual intake of dietary fat, 10 g being the threshold amount necessary to induce efficient GB emptying [10]. This has been clearly shown by Gebhard et al. [17], who compared two different regimens of 520 kcal (with ,2 g of fat) and 900 kcal (with 10 g of fat). GD developed in 66% of patients in the first group, who also showed severely reduced GB emptying (to an average of 35%), whereas GD developed in none of the patients in the second group, who showed less reduction in GB emptying (to an average of 66%). This aspect was further investigated by Festi et al. [16], who used two isocaloric regimens of |550 kcal each, with different amount of fat (3 vs. 12.2 g / day); as expected, a significant proportion of patients on the low fat schedule developed GD (54% vs. no case in the other group) and showed a marked reduction of GB emptying (which was normal in the high fat group). In a recent study of Zapata et al. [18], incidence of GD and pattern of GB emptying were similar in 12 obese subjects and 12 healthy females given a diet of 800–1200 kcal / day with 26 g of fat for 6 months. However, results are difficult to interpret due to the unusually high fat content and the fact that data analysis was limited to only six of the obese subjects.

population in central Italy, clearly indicated that hypertriglyceridaemia is an independent risk factor for GD; this has been confirmed in various other studies [22–24], although their conclusions have been challenged [25]. The exact mechanism by which hypertriglyceridaemia increases the risk of GD is still unclear, although patients with type IV hyperlipoproteinaemia abnormalities in synthesis, pool composition and enterohepatic dynamics of bile salts [26,27], including a deficient intestinal uptake [28], have been reported. Furthermore, it must be remembered that an increase in plasma triglyceride levels is a physiological P-P event whose duration could affect lithogenic potential. In addition to obesity and metabolic factors, attention has been given to a possible impairment of GB motility in diabetic subjects, mainly due to an underlying autonomic neuropathy. Once again, studies are difficult to compare due to their heterogeneity in terms of the methods of investigation, characteristics of the GB stimuli and differences in target population. As a consequence, there are conflicting data in relation to both the increase in GB fasting volume [29–36,38–40] and P-P GB contraction [31,33–41]. Difficulties in correctly interpreting the data concerning GB kinetics are mainly due to lack of patient stratification on the basis of the presence or absence of autonomic neuropathy that has been reported to decrease GB motility [31,35–39]. Other factors possibly involved in altered GB motility include a decrease in sensitivity of GB smooth muscle to P-P levels of plasma CCK [38], and / or a reduced number of CCK receptors on the GB wall [38]. The main data concerning GB motility in diabetic patients are listed in Table 2.

2. Diabetes A two- to three-fold increase in risk of cholesterol gallstones has been reported in diabetic patients [19–21]. There are two possibly related risk factors: obesity, the role of which has been discussed above, and hypertriglyceridaemia. Data from the MICOL study [19] of a large sample of subjects representative of the general

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3. Coeliac disease Impaired gallbladder [42–47], stomach [48,49] and small bowel motility [50] have been reported in patients

Table 2 GB fasting volume and P-P motility according to the technique and GB stimulus used Author [Ref.]

Patients (n)

Type of GB stimulus

Technique used

GB fasting volume

P-P GB motility a

Stone [37] Shreiner [41] Fiorucci [39] Hahm [31] Chapman [32] Palasciano [35] Shaw [40] Keshavarzian [33] Wedmann [34] Mitsukawa [38]

30 8 21 24 271 21 10 47 50 28

CCK CCK Solid Solid NR Solid Liquid Solid Liquid Solid

Scintigraphy Scintigraphy US US US US US US US US

NR NR ↑ ↑ ↑ ↑ NR ND ND NR

↓ ↓ ↓ ↓ NR ↓ ↓ ND ND ↓

ND, no significant differences; NR, not reported; US, ultrasound; ↓, decreased. a Versus control.

M. Fraquelli et al. / Digestive and Liver Disease 35 ( Suppl. 3) (2003) S12 –S16

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Table 3 Main results of the studies evaluating fasting GB volume and P-P motility in patients with CD Author [Ref.]

Patients (n)

Type of stimulus

Technique used

GB fasting volume

P-P GB a motility

Low Beer [43] Brown [45] Fraquelli [47] Maton [51] Delamarre [46]

18 8 10 8 4

CCK analogue CCK analogue Liquid Liquid Solid

Scintigraphy Scintigraphy US US US

NR NR ↑ NR NR

↓ ↓ ↓ ↓ ↓

NR, not reported; US, ultrasound; ↓, decreased. a Versus control.

with coeliac disease (CD), and attributed to a reduced secretion of enteric hormones [44,50] or decreased sensitivity to them [45]. For the purposes of this review, we will only consider GB motility. As shown in Table 3, a number of authors have reported a reduction both in absolute and net GB emptying in response to various stimuli in untreated coeliacs, a finding that may be due to altered secretion of different GI hormones, particularly CCK. As observed by some authors [42,44,51,52] and confirmed in one of our previous studies [47], P-P CCK levels are low in untreated coeliac patients despite the concomitant increase in the number of duodenal CCK secreting cells. As a consequence of the impaired lipolysis of exogenous fat, CCK cells are not adequately stimulated to release the hormone [53], and the consequent GB inertia also contributes toward impairment of small bowel transit time and enterohepatic circulation of bile salts. Furthermore, somatostatin (SS) secretion is altered in newly diagnosed coeliac patients, as we have demonstrated in a series of patients whose fasting SS levels were significantly higher than in controls. As previously reported by Sjolund et al. [54], this may be due to an increased number of SS secreting cells, which would account for the increase in baseline GB volume. Correlation between fasting SS levels and GB size has clearly been confirmed in patients affected by somatostatinoma or treated with SS or SS analogues [55,56]. We have also found increased serum neurotensin (NT) levels in untreated coeliac patients. The physiological P-P increase in this hormone is a reliable index of nutrient delivery to ileum [57], and may impair GB motility directly or indirectly by delaying gastric emptying, as previously reported [58]. Interestingly, the GI hormone abnormalities and their effects on GB, gastric and small bowel motility normalise completely after the successful administration of a gluten-free diet [44,47,48,59]. Overall, in all the clinical conditions examined here, interesting data have emerged from the evaluation of GB motility and / or pattern of GI hormones, although it would be advisable to standardise the techniques, types of stimuli and target populations.

Conflict of interest None declared.

List of abbreviations BMI, body mass index; CCK, cholecystokinin; GB, gallbladder; GD, gallstone disease; NT, neurotensin; P-P, postprandial.

References [1] Stampfer MJ, Maclure KM, Colditz GA, Manson JE, Willett WC. Risk of symptomatic gallstones in women with severe obesity. Am J Clin Nutr 1992;55:652–8. [2] Kodama H, Kono S, Todoroki I, Honjo S, Sakurai Y, Wakabayashi K, et al. Gallstone disease risk in relation to body mass index and waist-to-hip ratio in Japanese men. Int J Obes Relat Metab Disord 1999;23:211–6. [3] Bennion LJ, Grundy SM. Effects of obesity and caloric intake on biliary metabolism in man. J Clin Invest 1975;56:996–1011. [4] Palasciano G, Serio G, Portincasa P, Palmieri V, Fanelli M, Velardi A, et al. Gallbladder volume in adults, and relationship to age, body mass index and gallstones: a sonographic population study. Am J Gastroenterol 1992;87:493–7. [5] Hartz AJ, Rupley DC, Rimm AA. The association of girth measurement with disease in 32,856 women. Am J Epidemiol 1989;129:587–95. [6] Hendel HW, Hojgaard L, Andersen T, Pedersen BH, Paloheimo LI, Rehfeld JF, et al. Fasting gallbladder volume and lithogenicity in relation to glucose tolerance, total and intra-abdominal fat masses in obese non-diabetic subjects. Int J Obes Relat Metab Disord 1998;22:294–302. ¨ [7] Gielkens HA, Lam WF, Coenraad M, Frolich M, van Oostayen JA, Lamers BHW, et al. Effect of insulin on basal and cholecystokininstimulated gallbladder motility in humans. J Hepatol 1998;28:595– 602. [8] Marzio L, Capone F, Neri M, Mezzetti A, De Angelis C, Cuccurullo F. Gallbladder kinetics in obese patients: effect of a regular and low calorie meal. Dig Dis Sci 1988;33:4–9. [9] Acalovschi M, Badea R. Ultrasonographic study of gall-bladder emptying in obese patients. Int J Obes Relat Metab Disord 1992;16:313–5.

M. Fraquelli et al. / Digestive and Liver Disease 35 ( Suppl. 3) (2003) S12 –S16 [10] Stone BG, Ansel HJ, Peterson FJ, Gebhard RL. Gallbladder emptying stimuli in obese and normal weight subjects. Hepatology 1992;15:795–8. [11] Vezina WC, Paradis RL, Grace DM, Zimmer RA, Lamont DD, Rycroft KM, et al. Increased volume and decreased emptying of gallbladder in large (morbidly obese, tall normal and muscular normal) people. Gastroenterology 1990;98:1000–7. [12] Everhart JE. Contribution of obesity and weight loss to gallstone disease. Ann Intern Med 1993;119:1029–35. [13] Mazzella G, Bazzoli F, Festi D, Ronchi M, Aldini R, Roda A, et al. Comparative evaluation of chenodeoxycholic and ursodeoxycholic acids in obese patients. Effect of lipid metabolism during weight maintenance and weight reduction. Gastroenterology 1991;101:490– 6. [14] Marks JW, Bonorris GG, Albers G, Schoenfield LJ. The sequence of biliary events preceding the formation of gallstones in humans. Gastroenterology 1992;103:566–70. [15] Shiffman ML, Sugerman HJ, Kellum JM, Moore EW. Changes in gallbladder bile composition following gallstone formation and weight reduction. Gastroenterology 1992;103:214–21. [16] Festi D, Colecchia A, Orsini M, Sangermano A, Sottili S, Simoni P, et al. Gallbladder motility and gallstone formation in obese patients following very low calorie diets. Use it (fat) to lose it (well). Int J Obes 1998;22:592–600. [17] Gebhard RL, Prigge WF, Ansel HJ, Schlasner L, Ketover SR, Sande D, et al. The role of gallbladder emptying in gallstone formation during diet-induced rapid weight loss. Hepatology 1996;99:1779– 85. [18] Zapata R, Severin C, Manriquez M, Valdivieso V. Gallbladder motility and lithogenesis in obese patients during diet-induced weight loss. Dig Dis Sci 2000;45:421–8. [19] Attili AF, Capocaccia L, Carulli N, Festi D, Roda E, Barbara L, et al. Factors associated with gallstone disease in the MICOL experience. Hepatology 1997;26:809–18. [20] De Sanctis A, Attili AF, Ginanni Corradini S, Scafato E, Cantagalli A, De Luca C, et al. Gallstones and diabetes: a case-control study in a free-living population sample. Hepatology 1997;25:787–90. [21] Lieber MM. The incidence of gallstones and their correlation with other diseases. Ann Surg 1952;135:394–405. [22] the GREPCO Group, Angelico M. Relationships between serum lipids and cholelithiasis: observation in the GREPCO study. In: Capocaccia L, Ricci G, Angelico F, Angelico M, Attili AF, editors, Epidemiology and Prevention of Gallstone Disease, Lancaster: MTP Press, 1984, pp. 77–84. [23] Ahlberg J, Angelin B, Einarsson K, Hellstrom L, Leijd B. Prevalence of gallbladder disease in hyperlipoproteinaemia. Dig Dis Sci 1979;24:459–64. [24] Kadziolka R, Nilsson S, Schersten T. Prevalence of hyperlipoproteinaemia in men with gallstone disease. Scand J Gastroenterol 1977;12:353–5. [25] Barbara L, Sama C, Morselli-Labate AM, Taroni F, Rusticali AG, Festi D, et al. A population study on the prevalence of gallstone disease: the Sirmione study. Hepatology 1987;7:913–7. [26] Angelin B, Herson KS, Brunzell JD. Bile acid metabolism in hereditary forms of hypertriglyceridemia: evidence for an increased synthesis rate in monogenic familial hypertriglyceridemia. Proc Natl Acad Sci USA 1987;84:5434–8. [27] Angelin B, Einarsson L, Hellstrom K, Kallner M. Elimination of cholesterol in hyperlipoproteinaemia. Clin Sci Mol Med 1976;52:393–7. [28] Scragg RKR, Calvert GD, Oliver JR. Plasma lipids and insulin in gallstone disease: a case-control study. Br Med J 1984;289:521–5. [29] Braverman D. The lack of effect of metoclopramide on gallbladder volume and contraction in diabetic cholecystoparesis. Am J Gastroenterol 1986;15:535–9. [30] Kronert K, Gotz V, Reuland P, Luft D, Eggstein M. Gallbladder emptying in diabetic patients and control subjects assessed by

[31]

[32]

[33]

[34]

[35]

[36]

[37]

[38]

[39]

[40]

[41] [42]

[43]

[44]

[45]

[46]

[47]

[48]

[49]

[50]

[51]

S15

real-time ultrasonography and cholescintigraphy: a methodological comparison. Ultrasound Med Biol 1989;15:535–9. Hahm J, Park J, Park K, Ahn Y, Lee M, Park K. Gallbladder motility in diabetes mellitus using real time ultrasonography. Am J Gastroenterol 1996;91:2391–4. Chapman B, Chapman T, Frampton C, Chisholm RJ, Wilson IR, et al. Gallbladder volume: comparison of diabetics and controls. Dig Dis Sci 1992;37:1671–7. Keshavarzian A, Dunne M, Iber FL. Gallbladder volume and emptying in insulin-requiring male diabetics. Dig Dis Sci 1987;32:1089–97. Wedmann B, Droge C, Amoiridis G, Schmidt-Heinevetter G, Wegener M, Ricken D. Gallbladder motility in diabetic patients with and without cardiovascular neuropathy. Z Gastroenterol 1992;30:519–24. Palasciano G, Portincasa P, Belfiore A, Baldassarre G, Cignarelli M, Paternostro A, et al. Gallbladder volume and emptying in diabetics: the role of neuropathy and obesity. J Intern Med 1992;231:123–7. Catnach S, Ballinger A, Stevens M, Fairclough PD, Trembath RC, Drury PL, et al. Erythromicin induces supranormal gallbladder contraction in diabetic autonomic neuropathy. Gut 1993;34:1123–7. Stone B, Gavaler J, Belle S, Shreiner D, Peleman R, Sarva R, et al. Impairment of gallbladder emptying in diabetes mellitus. Gastroenterology 1988;95:170–6. Mitsukawa T, Takemura J, Ohgo S, Mizuta M, Ii T, Kuribayashi T, et al. Gallbladder function and plasma cholecystokinin levels in diabetes mellitus. Am J Gastroenterol 1990;85:981–5. Fiorucci S, Bosso R, Scionti L, Di Santo S, Annibale B, Delle Fave G, et al. Neurohumoral control of gallbladder motility in healthy subjects and in diabetics patients with or without autonomic neuropathy. Dig Dis Sci 1990;35:1089–97. Shaw S, Hajnal F, Lebovitz Y, Ralls P, Bauer M, Valenzuela J, et al. Gallbladder dysfunction in diabetes mellitus. Dig Dis Sci 1993;38:490–6. Shreiner D, Sarva R, Van Thiel D, Yingvorapant N. Gallbladder function in diabetic patients. J Nucl Med 1986;27:357–60. Low Beer TS, Harvey RF, Davies ER, Read AF. Abnormalities of serum cholecystokinin and gallbladder emptying in celiac disease. N Engl J Med 1975;292:961–3. Low Beer TS, Heaton KW, Heaton ST. Gallbladder inertia and sluggish enterohepatic circulation of bile salt in celiac disease. Lancet 1971;1:991–4. DiMagno EP, Go VLW, Summerskill WHJ. Impaired cholecystokinin-pancreozymin secretion, intraluminal dilution and maldigestion of fat in sprue. Gastroenterology 1972;63:25–32. Brown AM, Bradshaw MJ, Richardson R, et al. Pathogenesis of the impaired gallbladder contraction of coeliac disease. Gut 1987;28:1426–32. Delamarre J, Capron JP, Joly JP, Audebert M, Murat JL, Remond A, et al. Gallbladder inertia in celiac disease: ultrasonographic demonstration. Dig Dis Sci 1984;29:876–7. Fraquelli M, Bardella MT, Peracchi AM, Cesana BM, Bianchi PA, Conte D. Gallbladder emptying and somatostatin and cholecystokinin levels in celiac disease. Am J Gastroenterol 1999;94:1866–70. Bardella MT, Fraquelli M, Peracchi AM, Cesana BM, Bianchi PA, Conte D. Gastric emptying and plasma neurotensin levels in untreated celiac patients. Scand J Gastroenterol 2000;35:269–73. Usai P, Usai Satta P, Lai M, Corda MG, Piras E, Calcara E, et al. Autonomic dysfunction and upper digestive functional disorders in untreated adult coeliac disease. Eur J Clin Invest 1997;27:1009–15. Spiller RC, Frost PF, Stewart JS, Bloom SR, Silk DBA. Delayed postprandial plasma bile acid response in celiac patients with slow mouth–caecum transit. Clin Sci 1987;72:217–23. Maton PN, Selden AC, Fitzpareick ML, Chadwick VS. Defective gallbladder emptying and cholecystokinin release in celiac disease. Gastroenterology 1985;88:391–6.

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[52] Jansen JBMJ, Hopman WPM, Rosenbusch G. Plasma cholecystokinin and gallbladder responses to intraduodenal fat and intravenous cholecystokinin in patients with coeliac disease. Eur J Gastroenterol Hepatol 1992;4:349–53. [53] Hopman WPM, Rosenbusch G, Hectors MPC, Jansen JB. Effect of predigested fat on intestinal stimulation of plasma cholecystokinin and gallbladder motility in coeliac disease. Gut 1995;36:17–21. [54] Sjolund K, Alumets J, Berg NO, Hakanson R, Sundler F. Duodenal endocrine cells in adult coeliac disease. Gut 1979;20:547–52. [55] Krejs GJ, Orci L, Conlon JM, Ravazzola M, Davis GR, Raskin P, et al. Somatostatinoma syndrome: biochemical, morphologic and clinical features. N Engl J Med 1979;301:285.

[56] Redfern JS, Fortuner WJ. Octreotide-associated biliary tract dysfunction and gallstone formation: pathophysiology and management. Am J Gastroenterol 1995;90:1042–52. [57] Camilleri M, Balm RK, Low PA. Autonomic dysfunction in patients with chronic intestinal pseudo-obstruction. Clin Auton Res 1993;3:95–100. [58] Blackburn AM, Fletcher DR, Bloom SR, Christofides ND, Long RG, Fitzpatrick ML, et al. Effect of neurotensin on gastric function in man. Lancet 1980;i:987–9. [59] Masclee AAM, Jansen JBMJ, Driessen WMM, et al. Gallbladder sensitivity to cholecystokinin in coeliac disease. Scand J Gastroenterol 1991;26:1279–84.