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Fractionation of polysaccharides by gradient non-solvent precipitation: A review
Accepted Manuscript Fractionation of polysaccharides by gradient non-solvent precipitation: A review Xiuting Hu, H. Douglas Goff
PII:
S0924-2244(18)30149-3
DOI:
10.1016/j.tifs.2018.09.011
Reference:
TIFS 2318
To appear in:
Trends in Food Science & Technology
Received Date: 4 March 2018 Revised Date:
30 July 2018
Accepted Date: 9 September 2018
Please cite this article as: Hu, X., Goff, H.D., Fractionation of polysaccharides by gradient non-solvent precipitation: A review, Trends in Food Science & Technology (2018), doi: 10.1016/j.tifs.2018.09.011. This is a PDF file of an unedited manuscript that has been accepted for publication. As a service to our customers we are providing this early version of the manuscript. The manuscript will undergo copyediting, typesetting, and review of the resulting proof before it is published in its final form. 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.
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Fractionation of polysaccharides by gradient non-solvent precipitation: A review
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Xiuting Hua*, H. Douglas Goff b,**
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a
School of Food Science and Technology, Nanchang University, Nanchang 330047, China
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b
Department of food science, University of Guelph, Guelph, Ontario N1G2W1, Canada
* Corresponding author
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Xiuting Hu
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School of Food Science and Technology, Nanchang University
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Tel.: +86-791-88304753
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E-mail address: [email protected]
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H. Douglas Goff
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Department of Food Science, University of Guelph
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Tel.: +1- 519 824 4120
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E-mail address: [email protected]
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Abstract:
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Background Almost all natural polysaccharides have wide molecular weight distribution and the complex
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heterogeneous polysaccharides may also exhibit variations in proportions of sugar constituents,
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linkage type, degree and arrangement of branching or degree of substitution. The heterogeneity of
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molecular weight and chemical structure restricts basic research and application of
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polysaccharides. Therefore, it is meaningful to fractionate polysaccharides into fractions with high
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homogeneity in molecular weight and chemical structure.
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Scope and Approach
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Compared with chromatography and ultrafiltration, gradient non-solvent precipitation is
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inexpensive, has a wide application scope and can be easily scaled up or down as required.
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Therefore, this work reviews fractionation of polysaccharides by gradient non-solvent
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precipitation. Specifically, this work describes the commonly used non-solvents, fractionation
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mechanism of gradient non-solvent precipitation, how to establish the fractionation procedure,
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assessment of the fractionation effect and factors that affect fractionation.
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Key Findings and Conclusions
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This paper provides comprehensive and detailed directions for how to fractionate a new
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polysaccharide using this method. It is suggested to select a suitable non-solvent and establish the
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fractionation procedure according to the curve of the polysaccharide recovery as a function of the
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non-solvent concentration. Fractionation by gradient non-solvent precipitation is based on the
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difference in solubility of polysaccharides. Therefore, fractionation may be affected by the
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precipitation conditions and those factors that can affect the solubility of polysaccharides. During
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fractionation, those factors that negatively affect fractionation should be strictly controlled.
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Keywords: polysaccharide; fractionation; gradient precipitation; organic solvents; ammonium
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sulfate; polyethylene glycol
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1 Introduction Polysaccharides are widely distributed in plants, animals, fungi and microorganisms. They
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serve organisms in crucial functions, such as energy storage, structure and defense orientation.
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Natural polysaccharides and their derivatives are also widely used in food and pharmaceutical
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industries as the gelling agent, stabilizer, thickener or disintegrator. Polysaccharides are divided
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into homopolysaccharides and heteropolysaccharides. The former contains one kind of
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monosaccharide unit and the latter contains two or more kinds of monosaccharide units. Unlike
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small compounds made up of only one kind of molecule, polysaccharides consist of very different
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species. In the simplest case of linear homopolymers, those polysaccharides exhibit a wide
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distribution of molecular weight (chain length, or degree of polymerization). In addition to
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molecular weight, complex heteropolysaccharides may exhibit variations in proportions of sugar
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constituents, linkage type, or degree and arrangement of branching. In addition, the
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monosaccharide units of some polysaccharides may be sulfated, acetylated, methylated or
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substituted by other groups. Therefore, these polysaccharides may also have difference in the
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degree of substitution.
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Because relatively small differences in molecular weight and structure of polysaccharides
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may result in substantial differences in their physicochemical properties, the availability of
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samples with sufficiently high uniformity constitutes an indispensable requirement in the fields of
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basic research and for analytical purposes (Eckelt, Haase, Loske, & Wolf, 2004). In the former
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case, it is mandatory for the theoretical interpretation of measurements. In the latter, calibration of
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analytical methods often requires high uniformity standards. For instance, size exclusion
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chromatography (SEC) is frequently used for the measurement of molecular weight and molecular
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weight distribution of polymers (Wang, Wood, Huang, & Cui, 2003). Unless the system is
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molecular weight standards have to be used to calibrate the SEC columns. Pullulan and dextran
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are commercially available standards for polysaccharides. However, because the retention volume
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in SEC is dependent on hydrodynamic volume rather than molecular weight, the use of pullulan or
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dextran as standards can lead to inaccurate molecular weight determination of other
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polysaccharides. On the other hand, some fractions sometimes account for a quite low proportion
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in the polysaccharide sample, so it is difficult to identify these fractions by analyzing the whole
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polysaccharide sample. Fractionation can enrich these fractions. Therefore, it is necessary to
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fractionate them into more structurally homogeneous materials, particularly for unknown
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polysaccharides, when examining their molecular structures or structure-property relationships.
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Wide molecular weight distribution of polysaccharides also limits their industrial application. For
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instance, the molar mass of the hydroxyethyl starch generally used in clinical applications ranges
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40,000~450,000 g/mol and its molar degree of substitution ranges between 0.5 and 0.7 (Gosch,
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Haase, Wolf, & Kulicke, 2002). Hydroxyethyl starch of higher molar mass may induce
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anaphylactoid reactions. If the hydroxyethyl starch has an excessively low molar mass, it is
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excreted too quickly through the kidneys. There are considerable similar examples. Therefore, it is
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necessary to fractionate polysaccharides into fractions with high homogeneity.
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Fractionation of polysaccharides is mainly performed by chromatography, ultrafiltration and
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gradient non-solvent precipitation. Chromatography and ultrafiltration use columns and
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membranes to fractionate polysaccharides, respectively. Chromatography columns and filtration
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membranes have their specific molecular weight cut-off, and thus their ranges of application are
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limited. Fouling of chromatography columns and filtration membranes often result in their short
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industrialization of these two technologies. In addition, these methods are not suitable for
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large-scale preparations. Fractionation by gradient non-solvent precipitation means that gradual
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addition of non-solvent into the polysaccharide solution results in gradual precipitation of
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polysaccharides from the solution. This method is independent of special equipment and only
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requires simple equipment, such as stirred tanks and centrifuges, making it easily scalable up or
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down according to the need. Therefore, gradient non-solvent precipitation has the most potential
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for preparative fractionation of polysaccharides. In addition, this method has a large scope of
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application for different polysaccharides with different molecular weights. Therefore, fractionation
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of polysaccharides by gradient non-solvent precipitation is reviewed in this work.
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2 The non-solvent
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Usually, the solvent of polysaccharides is water. In an aqueous solution, polysaccharide
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molecules are linked with water molecules by hydrogen bonds, which keep polysaccharides
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soluble in water. The non-solvent can induce the precipitation of polysaccharides from the solution,
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thus the non-solvent is also named as the precipitant. The commonly used precipitants and the
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corresponding polysaccharides are summarized in Table 1. The precipitants include organic
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solvents (methanol, ethanol, isopropanol, acetone and 1-butanol), ammonium sulfate ((NH4)2SO4)
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and polyethylene glycol (PEG).
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Different from other organic solvents, 1-butanol can selectively precipitate amylose due to
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the formation of the amylose-1-butanol complex (Schoch, 1942). Therefore, 1-butanol can be
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exclusively used to fractionate starch into amylose and amylopectin. However, 1-butanol cannot
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fractionate other polysaccharides. Hence, fractionation by 1-butanol is not discussed in this paper.
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agent. These organic solvents have much lower dielectric constant than water. Adding organic
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solvents can lower the dielectric constant of the polysaccharide solution and promote
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intra-molecular associations of water-soluble polysaccharides through competition for water, thus
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inducing conformational changes, aggregation and precipitation of the polysaccharides (Jian, et al.,
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2014). In other words, organic solvents decrease the polarity of water to precipitate
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polysaccharides, because organic solvents have much lower polarity than water (Guo, Meng, Tang,
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et al., 2016). According to the “like dissolves like” principle, the polysaccharides that are initially
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soluble will be eventually precipitated if enough organic solvents are added to decrease the
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polarity of water. The biggest difference of these organic solvents is the dielectric constant (or
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polarity) and their dielectric constant (or polarity) is in the order of methanol > ethanol >
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isopropanol > acetone. Therefore, the precipitation efficiency is in the order of methanol < ethanol
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< isopropanol < acetone. Among these precipitants, ethanol is the most widely used due to its
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safety and food purposes.
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Although the mechanism by which (NH4)2SO4 precipitates polysaccharides is not reported, it
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can be inferred that it is similar to the mechanism by which (NH4)2SO4 precipitates proteins. In an
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aqueous solution, the polysaccharide exposes its polar residues on the surface to maximize the
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contact with water molecules (Huang, et al., 2013). Water molecules bind to the surface of the
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biopolymer and form a hydration layer, which is essential to maintain the solubility and to prevent
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the contact and aggregation of the polysaccharide molecules. The electrostatic repulsion of the
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same charges in the charged polysaccharides also facilitates the interaction between the
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polysaccharides and water. When NH4+ and SO42− ions are added into the aqueous polysaccharide
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hydration layer, facilitating the interactions between the polysaccharide molecules to form
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aggregates and precipitate. In addition, they are attracted to the opposite charges evident on the
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polysaccharide. This attraction of opposite charges also leads to aggregation and precipitation of
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polysaccharides.
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Two chemically different water-soluble polymers are often incompatible in aqueous solutions.
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PEG is incompatible with dextran or dextrin. When the PEG concentration reaches the limiting
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value, phase separation happens and dextran or dextrin is precipitated from the solution. In
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summary, PEG precipitates dextran or dextrin based on their incompatibility. In addition to
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dextran and dextrin, PEG has the potential to fractionally precipitate other polysaccharides, since
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incompatibility widely exists between two chemically different water-soluble polymers. Actually,
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PEG precipitation has been widely used to purify proteins (Atha & Ingham, 1981;
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Hammerschmidt, Hobiger, & Jungbauer, 2016; Sim, et al., 2012).
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3 The principle of fractionation by gradient non-solvent precipitation
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Fractionation by gradient non-solvent precipitation is based on phase separation of
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polysaccharide solutions. Polysaccharides of different molecular weights or chemical structures
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have different solubility. Adding small amount of non-solvent initially leads to the precipitation of
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the polysaccharides with low solubility and subsequent addition of non-solvent gradually
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precipitates the polysaccharides with relatively high solubility, thereby achieving fractional
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precipitation of polysaccharides based on differential solubility. Generally, the solubility of
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polysaccharide is negatively correlated to its molecular weight (Hu et al., 2015; Hu, Liu, et al.,
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2017; Hu, Wang, et al., 2017). Therefore, gradient non-solvent precipitation often induces
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addition to the molecular weight, most polysaccharides exhibit variations in proportions of sugar
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constituents, linkage type, degree and arrangement of branching, and/or degree of substitution,
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which also result in differential solubility (Izydorczyk & Biliaderis, 1996). Therefore, the mode of
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fractionation is governed by not only the molecular weight but also the structural characteristics of
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polysaccharides. Generally, higher precipitant concentration is required to precipitate the
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polysaccharides with the structure characteristics that result in better solubility. For example, when
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galactomannan was fractionated by gradient (NH4)2SO4 precipitation, fractions precipitated at the
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lower saturation level of (NH4)2SO4 had less substituted mannan backbone compared with those
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obtained at a higher salt concentration (Izydorczyk & Biliaderis, 1996). It was also found that the
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less branched hemicelluloses were precipitated at lower ethanol percentages and more branched
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hemicelluloses were obtained at higher ethanol concentrations (Bian et al, 2010). In general,
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depending on the polysaccharide type, various factors, such as high molecular weight, low
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branching levels and high substitution by hydrophobic groups, favor precipitation of
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polysaccharides at low non-solvent concentrations.
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4 Establishment of the fractionation procedure
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Gradient non-solvent precipitation is often carried out as follows (Fig. 2). Non-solvent is
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uniformly added to the polysaccharide solution. Afterward, the solution is held for a certain period
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of time and then centrifuged to obtain the supernatant and precipitate. The residual non-solvent in
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the polysaccharide precipitate should be removed. Organic solvents can be removed by drying.
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After fractionation by (NH4)2SO4, the residual (NH4)2SO4 in the polysaccharide is often removed
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by dialysis. On the other hand, traces of PEG in the polysaccharide precipitate are often removed
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non-solvent into the obtained supernatant, another polysaccharide fraction can be precipitated and
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be designated as the 2nd fraction. The process of graded precipitation can proceed further to obtain
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more fractions. The final supernatant is usually abandoned. In theory, the polysaccharides in the
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final supernatant have high dispersity, since different polysaccharide species that are not
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precipitated are left in the supernatant. In addition, it takes time and energy to remove the
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cumulative non-solvents.
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The stepwise precipitant concentrations used to fractionally precipitate polysaccharides are
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the key of the fractionation procedure. A suitable initial precipitant concentration helps to save
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fractionation time. In order to save time and cost, it is expected to achieve the highest
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polysaccharide yield by using the lowest dose of the precipitant. However, it seems that
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polysaccharides cannot be completely precipitated from the solution, partially because there are
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fractions which are soluble at high precipitant concentrations. Therefore, most of the reports try to
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obtain the best fractionation effect rather than the biggest polysaccharide yield. As is shown in
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Table 2, the final alcohol concentration reached about 80% (v/v) in most cases. Although the
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alcohol concentration was high, the polysaccharide recovery was often less than 90%. One reason
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for this result might be that the parent polysaccharides usually contained large amount of
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impurities. However, the ethanol concentration of 33.3% or the isopropanol concentration of
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28.6% resulted in about 90% galactomannan recovery (Jian, et al., 2014). This may be due to the
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fact that galactomannan had very large molecular weight, which was confirmed by the result that
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the galactomannan recovery was positively correlated with the molecular weight. When
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fractionating sugar beet pectin, the highest isopropanol concentration was also very low, about
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beet pectin. Specifically, sugar beet pectin contained high amount of hydrophobic acetyl groups,
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ferulic acids and proteins. In addition, the fractionation procedures in different studies were
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diverse. A previous report that investigated the effect of structural diversity on ethanol
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concentration of precipitating polysaccharide also suggested that the ethanol concentration must
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be individually optimized for each type of polysaccharide during ethanol precipitation (Xu, et al.,
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2014). Different reports even used different non-solvent concentrations to fractionate the same
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polysaccharides. Therefore, it is difficult to select non-solvent concentrations for fractionating new
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polysaccharides according to the previous reports. It was suggested that the non-solvent
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concentrations could be selected based on the curves of the polysaccharide yield as a function of
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alcohol concentration (Hu, et al., 2015). Hu et al. first precipitated dextrin solutions using different
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alcohol concentrations to obtain the curves of the dextrin yield as a function of alcohol
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concentration. According to these curves, the dextrin yield did not significantly increase once the
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alcohol concentration was 86.7% (v/v). Therefore, fractionation was ended when the alcohol
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concentration reached 86.7%. When the alcohol concentration was 33.3%, the dextrin yield
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reached more than 30%. Therefore, the fractionation started from the alcohol concentration at
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20.0%. On the other hand, Gonzaga et al. added ethanol into the polysaccharide solution until the
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solution became turbid and stable to obtain the fractions (Gonzaga, et al., 2005). In addition to
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fractionation, gradient alcohol precipitation can be used to purify polysaccharides. For instance,
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heparin, dermatan sulfate and chondroitin sulfate in mixtures were successfully separated by
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sequential precipitation with methanol, ethanol or propanol (Volpi, 1996). Similarly, it was found
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that keratan sulfate could be precipitated prior to chondroitin sulfate (Galeotti, Maccari, & Volpi,
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2014). Therefore, keratan sulfate in chondroitin sulfate samples could be selectively removed by
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sequential precipitation with ethanol. When (NH4)2SO4 is used to fractionate polysaccharides, the (NH4)2SO4 concentration is often
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characterized by its saturation level. It seemed that (NH4)2SO4 had higher precipitation ability on
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glucan than other kinds of polysaccharides. Li et al. reported that β-glucans could be precipitated
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at a much lower saturation level of (NH4)2SO4 than arabinoxylans (Li, et al., 2006). Based on this
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principle, wheat β-glucan was separated from wheat arabinoxylan by gradient (NH4)2SO4
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precipitation.
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In summary, the precipitation efficiency of organic solvents is the lowest, partially because
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they are liquid. Compared with addition of solid (NH4)2SO4 and PEG, addition of equal organic
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solvents greatly increases the volume of the polysaccharide solution and decreases the
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polysaccharide concentration. To fractionate a new polysaccharide, it is suggested to first obtain
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the curve of the polysaccharide recovery as a function of the non-solvent concentration and then
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establish the fractionation procedure according to the curve.
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5 Assessment of the fractionation effect
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Sometimes, fractionation of polysaccharides just helps to enrich fractions and characterize
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polysaccharides. In this case, the fractionation effect is not assessed. Sometimes, the aim of
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fractionation is to obtain fractions with high homogeneity. Afterward, different fractions are used
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for different specific purposes. In this case, the molecular weight homogeneity and structural
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homogeneity of fractions obtained by fractionation should be determined to assess the
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fractionation effect. The homogeneity of molecular weight could be indicated by the
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molecular-weight dispersity (DM) (Stepto, 2010). The DM is calculated as the ratio of the
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the polysaccharides is larger than the Mn. Therefore, a lower DM indicates a narrower molecular
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weight distribution of the polysaccharides. When most of fractions obtained by fractionation have
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smaller DM than the parent polysaccharide, the fractionation is considered to be successful. One
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sample is always fractionated into several fractions, and different fractionation conditions always
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result in different mass distribution and molecular weight distribution of fractions. Therefore, the
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average molecular-weight dispersity (DMa) was defined as follows to assess the fractionation
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effect:
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DMa =
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where DMa was the average dispersity of the fractions in one group, DMi was the dispersity of the
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ith fraction, and the Xi was the mass fraction of the ith fraction (Hu, et al., 2016; Hu, Wang, et al.,
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2017). The lowest DMa indicated the best fractionation effect. However, structural homogeneity,
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including proportions of sugar constituents, linkage type, degree and arrangement of branching,
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and the degree of substitution, is difficult to assess and so far no related research is reported.
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6 Factors that affect fractionation
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In theory, fractionation by gradient non-solvent precipitation is affected by the precipitation
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conditions and those factors which affect the solubility of polysaccharides. The molecular weight
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of polysaccharide affects its solubility, so it also affects fractionation. It was found that the higher
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the level of high-molecular-weight dextrin, the broader the molecular weight distribution of the
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different dextrin fractions (Gelders, et al., 2003). Definitely, the effect of the molecular weight and
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structure of polysaccharides on fractionation cannot be eliminated. Therefore, more effort should
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be made to eliminate the negative effect of the external factors. The external factors are as follows:
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6.1 The rate of adding the precipitant It is easy to understand that the rate of adding the precipitant affects the precipitation process,
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particularly gradient precipitation during which limited precipitants are used to precipitate the
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polysaccharides. It was reported that the dextrin yield was higher when alcohol was quickly added
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than when it was slowly added (Hu, et al., 2015). It was postulated that adding alcohol fast
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resulted in extremely high alcohol concentration in certain parts of the dextrin solution, thus
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resulting in co-precipitation of the dextrin. As a result, the rate of adding alcohol should be
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carefully controlled during fractionation of dextrin by gradient alcohol precipitation. Similar
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phenomena occur to precipitation by (NH4)2SO4. Therefore, (NH4)2SO4 is often ground into
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powders. Alternatively, a saturated (NH4)2SO4 solution is used to avoid extremely high (NH4)2SO4
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concentration in certain parts. Similarly, (NH4)2SO4 powder or solution should be slowly added
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into
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PEG-polysaccharide-water system over the phase separation temperature. On the other hand, PEG
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is not quickly dissolved in water like these organic solvents and (NH4)2SO4. Therefore, combined
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with heating and stirring, quick addition of PEG is feasible during fractionation by PEG (Hu, et al.,
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2016). Alternatively, a PEG solution may be used in future.
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6.2 The precipitant
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Due to non-specificity, the three types of precipitants can be widely used to fractionate
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different kinds of polysaccharides. Basedow & Ebert used ethanol and PEG to fractionate dextran
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and found that the fractionation results of the two precipitants had no significant difference
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(Basedow & Ebert, 1979). However, Hu et al. found gradient alcohol precipitation had better
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In addition, the fractionation effect of alcohols was in the order of methanol > ethanol >
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isopropanol, while the precipitation efficiency was in the reverse order (Hu, et al., 2015). With
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regard to the choice of non-solvent, it should be noted that the non-solvent cannot have very
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strong precipitation ability (Zhang, et al., 2011). Otherwise, the fractionation will be difficult to
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control. For example, if one polysaccharide can be completely precipitated by adding ethanol at
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the concentration of 5% (v/v), it is almost impossible to control such a fractionation process. A
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suitable non-solvent is the one that can provide a board range of concentration to use. In this case,
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it is easy to control the fractionation process and adjust the non-solvent concentration for best
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fractionation. The suitable non-solvent may also be found from the curves of the polysaccharide
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recovery as a function of the non-solvent concentration.
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6.3 The precipitation temperature
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The precipitation temperature mainly affects the precipitation efficiency. Low fractionation
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temperature decreases the polarity of solvents and solubility of polysaccharides, thus improving
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the precipitation efficiency. Because the precipitation efficiency of organic solvents is relatively
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low, it is suggested to preform fractionation by gradient organic solvent precipitation at low
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temperature (Gelders, et al., 2003). Therefore, fractionation by organic solvents is often performed
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at 4 oC. However, the solubility of (NH4)2SO4 and PEG is low at low temperature and their
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precipitation efficiency is relatively high at room temperature. Therefore, fractionation by
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(NH4)2SO4 and PEG is often carried out at room temperature.
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6.4 The precipitation time
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The precipitation time may affect the polysaccharide recovery. It was found that the solubility
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quickly finished within minutes (Xu, et al., 2014). Similarly, it was inferred that precipitation of
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polysaccharides by (NH4)2SO4 was quickly finished. However, after the previous studies usually
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kept the polysaccharide solution added with organic solvents or (NH4)2SO4 at the precipitation
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temperature for 1 h or overnight to fully precipitate the polysaccharides. The phase separation of
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the polymer solution induced by another polymer is very slow. Therefore, the precipitation time of
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gradient PEG precipitation was 24 h (Hu, et al., 2016; Hu, Wang, et al., 2017).
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6.5 The initial polysaccharide concentration
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As stated above, fractionation by gradient non-solvent precipitation is based on differential
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solubility of the polysaccharides. The solubility of polysaccharides is dependent on their
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molecular weight and chemical structure. Undoubtedly, the polysaccharide solubility also depends
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on its concentration. Therefore, the initial polysaccharide concentration may affect fractionation of
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polysaccharide. The key of graded precipitation is to avoid co-precipitation of different
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components. Therefore, the polysaccharide concentration cannot be too high, as co-precipitation
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easily happens at high concentration, especially in the first fraction. The fractionation result is
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usually better when the concentration of the polysaccharide solution is lower. But if the
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polysaccharide concentration is too low, the recovery of polysaccharide will decrease and the
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consumption of the non-solvent will greatly increase. In general, the initial polysaccharide
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concentration often ranges from 0.1% to 4% (w/v), which is usually negatively correlated with the
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molecular weight. However, the most suitable initial concentration may depend on many factors.
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Hu et al. found that when dextrin was fractionally precipitated by ethanol, the optimal initial
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concentration was in the range of 1.8%–2.7% (Hu, et al., 2015). However, when fractionating the
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same dextrin by gradient PEG precipitation, the initial dextrin concentration, which ranged from
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0.9% to 3.6%, did not affect the DMa of the dextrin fractions (Hu, Wang, et al., 2017).
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6.6 The pH Hydroxyl groups in polysaccharide chain are ionized at high pH (Hedayati, Shahidi,
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Koocheki, Farahnaky, & Majzoobi, 2016). Alkali can also break the intermolecular hydrogen
335
bonds of polysaccharide. Thus, pH can affect the polysaccharide solubility. In addition, the
336
solubility of charged polysaccharides is more sensitive to pH, because pH can affect the ionization
337
of dissociable groups in charged polysaccharides, such as carboxyl groups and amino groups. It
338
was also reported that pH had a significant effect on the alcoholic precipitation of sugar beet
339
pectin (Guo, Meng, Tang, et al., 2016). Therefore, pH is likely to affect fractionation of
340
polysaccharides. Hu et al. found that neutral environment was the most suitable for fractionation
341
of dextrin by gradient alcohol precipitation, while a weakly alkaline environment was optimal for
342
fractionation of dextrin by gradient PEG precipitation (Hu, Liu, et al., 2017; Hu, Wang, et al.,
343
2017). The pH could change the solubility of dextrin in alcohol or PEG solution. Theoretically, the
344
most suitable pH for dextrin fractionation was the one that could provide the greatest solubility
345
difference between high-molecular-weight dextrin and low-molecular-weight dextrin. Therefore, it
346
was likely that neutral and slightly alkaline environment provided the greatest solubility difference
347
between high-molecular-weight dextrin and low-molecular-weight dextrin in the alcohol and PEG
348
solution, respectively. However, the effect of pH on fractionation of other polysaccharides has not
349
been reported yet. Previous reports often fractionated polysaccharides in a neutral environment.
350
6.7 Other factors
351
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When alcohol was used as the precipitant, salt also affected fractionation (Hu, Liu, et al.,
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ACCEPTED MANUSCRIPT 2017). When dextrin was fractionated in KCl solutions, salt was co-precipitated with dextrin. KCl
353
resulted in earlier precipitation of dextrin compared to salt-free solution and co-precipitation of
354
dextrin, which was in accordance with the conclusion that salts decreased the solubility of starch
355
(Zhou, et al., 2014). In this case, salt might decrease the solubility difference of dextrin with
356
different sizes, thus negatively affecting fractionation of dextrin. A similar phenomenon may occur
357
to other polysaccharides. In addition, the cation-pectin electrostatic interaction significantly
358
weakened the hydration degree of sugar beet pectin, especially when divalent cations were used,
359
and the combined effect of added counter cations and ethanol led to a significant increase in the
360
precipitation of negatively-charged sugar beet pectin (Guo, Zhang, Meng, & Yu, 2017). Therefore,
361
divalent cations may affect fractionation of pectin and other negatively charged polysaccharides
362
through electrostatic interaction.
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When PEG was used as the precipitant, fractionation was also affected by the molecular
364
weight and molecular weight distribution of PEG (Hu, et al., 2016). PEG with high molecular
365
weight (over 20000 Da) could induce very high viscosity of the solution, which impeded
366
fractionation. Furthermore, fractionation was best accomplished by the most narrowly-distributed
367
PEG.
368
7 Conclusions
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Gradient non-solvent precipitation provides a simple and facile way for preparative
370
fractionation of polysaccharides. The non-specificity of the non-solvents makes this method
371
suitable for fractionating almost all kinds of polysaccharides. The fractionation result is affected
372
by various factors and difficult to predict. In theory, enlarging the solubility difference among
373
polysaccharides facilitates fractionation by gradient precipitation. However, the non-specificity of
18
ACCEPTED MANUSCRIPT these precipitants makes it difficult to obtain products with enough uniformity. Therefore, it is still
375
a long-standing challenge to get access to structurally-homogeneous polysaccharides, especially
376
polysaccharides with high molecular weight. Repeated fractionation by one non-solvent or
377
combination of different non-solvents may help to obtain polysaccharides with high uniformity. To
378
extend industrial application of this method, further research is needed to shorten the fractionation
379
time and design special equipment for improving its continuity of operation.
380
Acknowledgements
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This work was supported by the National Natural Science Foundation of China (31601425)
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and Project of Jiangxi Province Education Department (GJJ160187).
383
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571
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573
Fig. 1 Schematic representation of fractionating polysaccharides by gradient non-solvent
574
precipitation in the descending order of molecular weight.
575
Fig. 2 The fractionation procedure by gradient non-solvent precipitation.
AC C
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Table 1 The commonly used precipitants and the corresponding polysaccharides. Polysaccharide
Reference
Methanol
Dextran
John Eckelt, Sugaya, & Wolf, 2006; Zief, Brunner, & Metzendorf, 1955
Dextrin
Bertoft, 1989; Gelders, Bijnens, Loosveld, Vidts, & Delcour, 2003; Hu, Liu, Jin, & Tian,
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Precipitant
2015
Basedow & Ebert, 1979; Neuchl & Mersmann, 1995, 1996
Dextrin
Defloor , Vandenreyken, Grobet, & Delcour, 1998; Frigard, Andersson, & Aman, 2002;
TE D
Dextran
Gelders, et al., 2003; Hu, Liu, Jin, & Tian, 2017; Hu, et al., 2015
Arabinan
Dervilly, Saulnier, Roger, & Thibault, 2000
EP
Wheat arabinoxylan
AC C
Ethanol
Cardoso, Silva, & Coimbra, 2002
Polysaccharides from Agaricus blazei Murill fructan
Gonzaga, Ricardo, Heatley, & Soares, 2005
Fructan
Paseephol, Small, & Sherkat, 2007; Pourfarzad, Habibi Najafi, Haddad Khodaparast, Hassanzadeh Khayyat, & Malekpour, 2014
ACCEPTED MANUSCRIPT
Bian, Peng, Peng, Xu, & Sun, 2010; Li, et al., 2016; Peng, et al., 2009; Peng, et al., 2010;
RI PT
Hemicellulose
Peng, et al., 2013; Peng, Peng, Bian, Xu, & Sun, 2011; Shi, Yang, Lin, & Peng, 2013;
SC
Xue, Wen, Xu, & Sun, 2012 Kang, et al., 2011
Exopolysaccharides from Cordyceps sinensis fungus
Huang, Siu, Wang, Cheung, & Wu, 2013
Polysaccharides
Zha, et al., 2012
from
Laminaria
japonica
Jian, et al., 2014
Pectin
Guo, Meng, Zhu, et al., 2016
Lycium
barbarum
AC C
from
Feng, Yin, Nie, Wan, & Xie, 2016
EP
Polysaccharides from Cassia obtusifolia Polysaccharides
TE D
Galactomannan gum
M AN U
Gum ghatti
Gong, et al., 2017
Polysaccharides from Moringaoleifera Lam. Leaves
Chen, Zhang, Huang, Fu, & Liu, 2017
Glucan
Wang, et al., 2017
Polysaccharide
form
Polyporus
umbellatus He, et al., 2017
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Li, Wang, Zheng, & Li, 2017
Dextran
Neuchl & Mersmann, 1996
Dextrin
Gelders, et al., 2003; Hu, et al., 2015
Galactomannan gum
Jian, et al., 2014
Pectin
Karnik, Jung, Hawking, & Wicker, 2016; Karnik & Wicker, 2018; Nagel, et al., 2017
Acetone
Pullulan
John Eckelt, et al., 2006
1-Butanol
Starch
Cornell, McGrane, & Melbourne, 1999; Klucinec & Thompson, 1998; Li & Zhu, 2018;
SC
M AN U
TE D
Isopropanol
RI PT
Polysaccharides from Gynura procumbens
Schoch, 1942 Izydorczyk & Biliaderis, 1992
EP
Arabinoxylan Galactomannan Glucan
AC C
(NH4)2SO4
Mushroom polysaccharides
Izydorczyk, &Biliaderis, 1996 Izydorczyk, Biliaderis, Macri, & MacGregor, 1998; Li, Cui, & Kakuda, 2006; Ragaee, et al., 2008; Wang, et al., 2003 Zhang, et al., 2011
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Guan, et al., 2015; Peng, et al., 2012
Polysaccharide from leaf skin of Aloe barbadensis
Shi, et al., 2017
RI PT
Hemicellulose
Basedow & Ebert, 1979
Dextrin
Hu, Liu, Jin, & Tian, 2016; Hu, Wang, Liu, Jin, & Tian, 2017
EP
TE D
M AN U
Dextran
AC C
PEG
SC
Miller
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Non-solvent concentrations
Polysaccharide
Methanol (v/v)
20%, 33%, 50%, 66.7%, 75%, 80% and 83%
Dextrin
Ethanol (v/v)
20%, 33%, 50%, 66.7%, 75%, 80% and 83%
Dextrin
20%, 30%, 40%, 50%, 60% and 70% 50%, 65% and 80%
Reference Hu, et al., 2015 Hu, et al., 2015; Hu, Liu, et al., 2017
Arabinoxylan
Dervilly, et al., 2000
Arabinan
Cardoso, et al., 2002
Hemicellulose
Peng, et al., 2009; Peng, et al., 2010
TE D
15%, 30% and 60%
SC
Non-solvent
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Table 2 Examples of the non-solvent concentrations used during gradient precipitation.
Hemicellulose
Bian, et al., 2010
Hemicellulose
Peng, et al., 2011
Hemicellulose
Xue, et al., 2012
Hemicellulose
Peng, et al., 2013
50%, 67%, 75%, 83% and 88%
Hemicellulose
Shi, et al., 2013
15%, 30%, 45% and 60%
Hemicellulose
Li, et al., 2016
10%, 20%, 30%, 45%, 60% and 80%
EP
15%, 30%, 45%, 60% and 75%
20%, 40%, 60% and 80%
AC C
15%, 60% and 90%
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17%, 29%, 50%, 67% and 84%
Polysaccharide from Cordyceps sinensis
Huang, et al., 2013
40%, 60% and 80%
Polysaccharide from Laminaria japonica
Zha, et al., 2012
23.1%, 28.6% and 33.3%
Galactomannan gum
Jian, et al., 2014
50%, 67%, 71%, 75%, 78% and 80%
Pectin
Guo, Meng, Zhu, et al., 2016
Polysaccharide from Lycium barbarum
Gong, et al., 2017
Polysaccharide from Moringaoleifera Lam
Chen, et al., 2017
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Gum ghatti
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50%, 65% and 80%
30%, 50% and 70%
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40%, 60% and 80%
Glucan
Wang, et al., 2017
Polysaccharide from Gynura procumbens
Li, et al., 2017
Dextrin
Hu, et al., 2015
Galactomannan
Jian, et al., 2014
10%, 18%, 25%, 31%, 36% and 40%
Sugar beet pectin
Karnik, et al., 2016
10%, 18%, 25% and 31%
Sugar beet pectin
Karnik & Wicker, 2018
30%, 50% and 70%
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20%, 40%, 60% and 80% 20%, 33%, 50%, 66.7%, 75%, 80% and 83%
(v/v)
16.7%, 23.1% and 28.6%
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Isopropanol
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Arabinoxylan
saturation level
20%, 30%, 45%, 80% and 100%
Galactomannan
70%, 80% and 100%
Galactomannan
30%, 35%, 40% and 50%
Glucan
15%, 15.5%, 16%, 16.3%, 16.6%, 17.2% and 21% 15.5%, 16.7%, 17.8%, 18.3%, 20%, 21.1% and 24%
and 33.5%
PEG
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5%, 15%, 25%, 40%, 55% and 70%
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16.4%, 16.8%,17.5%, 18.5%, 19.5%, 23.2%, 28.5%
the initial addition 5 g, stepwise 5 g, the final addition 80 g (For 100 mL solution)
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Izydorczyk, &Biliaderis, 1996 Izydorczyk, &Biliaderis, 1996 Izydorczyk, et al., 1998
Glucan
Wang, et al., 2003
Glucan
Wang, et al., 2003
Glucan
Li, et al., 2006
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16.2%, 17.01%, 18.01%, 19.44%, 24% and 40%
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60%, 70%, 80% and 95%
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Izydorczyk & Biliaderis, 1992
(NH4)2SO4
Glucan
Ragaee, et al., 2008
Polysaccharide from Aloe barbadensis Miller
Guan, et al., 2015
Dextrin
Hu, et al., 2016; Hu, Wang, et al., 2017
ACCEPTED MANUSCRIPT Fig. 1 Schematic representation of fractionating polysaccharides by gradient non-solvent
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precipitation in the descending order of molecular weight.
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Fig. 2 The fractionation procedure by gradient non-solvent precipitation.
ACCEPTED MANUSCRIPT Gradient precipitation is based on solubility differences of polysaccharides. Polysaccharides are generally precipitated in descending order of molecular weight. Non-solvents of polysaccharides mainly include organic solvents, (NH4)2SO4 and PEG.
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Fractionation of polysaccharides by this method is affected by various factors.
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PII:
S0924-2244(18)30149-3
DOI:
10.1016/j.tifs.2018.09.011
Reference:
TIFS 2318
To appear in:
Trends in Food Science & Technology
Received Date: 4 March 2018 Revised Date:
30 July 2018
Accepted Date: 9 September 2018
Please cite this article as: Hu, X., Goff, H.D., Fractionation of polysaccharides by gradient non-solvent precipitation: A review, Trends in Food Science & Technology (2018), doi: 10.1016/j.tifs.2018.09.011. This is a PDF file of an unedited manuscript that has been accepted for publication. As a service to our customers we are providing this early version of the manuscript. The manuscript will undergo copyediting, typesetting, and review of the resulting proof before it is published in its final form. 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.
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Fractionation of polysaccharides by gradient non-solvent precipitation: A review
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Xiuting Hua*, H. Douglas Goff b,**
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a
School of Food Science and Technology, Nanchang University, Nanchang 330047, China
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b
Department of food science, University of Guelph, Guelph, Ontario N1G2W1, Canada
* Corresponding author
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Xiuting Hu
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School of Food Science and Technology, Nanchang University
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Tel.: +86-791-88304753
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E-mail address: [email protected]
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H. Douglas Goff
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Department of Food Science, University of Guelph
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Tel.: +1- 519 824 4120
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E-mail address: [email protected]
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Abstract:
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Background Almost all natural polysaccharides have wide molecular weight distribution and the complex
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heterogeneous polysaccharides may also exhibit variations in proportions of sugar constituents,
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linkage type, degree and arrangement of branching or degree of substitution. The heterogeneity of
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molecular weight and chemical structure restricts basic research and application of
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polysaccharides. Therefore, it is meaningful to fractionate polysaccharides into fractions with high
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homogeneity in molecular weight and chemical structure.
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Scope and Approach
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Compared with chromatography and ultrafiltration, gradient non-solvent precipitation is
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inexpensive, has a wide application scope and can be easily scaled up or down as required.
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Therefore, this work reviews fractionation of polysaccharides by gradient non-solvent
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precipitation. Specifically, this work describes the commonly used non-solvents, fractionation
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mechanism of gradient non-solvent precipitation, how to establish the fractionation procedure,
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assessment of the fractionation effect and factors that affect fractionation.
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Key Findings and Conclusions
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This paper provides comprehensive and detailed directions for how to fractionate a new
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polysaccharide using this method. It is suggested to select a suitable non-solvent and establish the
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fractionation procedure according to the curve of the polysaccharide recovery as a function of the
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non-solvent concentration. Fractionation by gradient non-solvent precipitation is based on the
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difference in solubility of polysaccharides. Therefore, fractionation may be affected by the
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precipitation conditions and those factors that can affect the solubility of polysaccharides. During
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fractionation, those factors that negatively affect fractionation should be strictly controlled.
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Keywords: polysaccharide; fractionation; gradient precipitation; organic solvents; ammonium
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sulfate; polyethylene glycol
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1 Introduction Polysaccharides are widely distributed in plants, animals, fungi and microorganisms. They
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serve organisms in crucial functions, such as energy storage, structure and defense orientation.
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Natural polysaccharides and their derivatives are also widely used in food and pharmaceutical
48
industries as the gelling agent, stabilizer, thickener or disintegrator. Polysaccharides are divided
49
into homopolysaccharides and heteropolysaccharides. The former contains one kind of
50
monosaccharide unit and the latter contains two or more kinds of monosaccharide units. Unlike
51
small compounds made up of only one kind of molecule, polysaccharides consist of very different
52
species. In the simplest case of linear homopolymers, those polysaccharides exhibit a wide
53
distribution of molecular weight (chain length, or degree of polymerization). In addition to
54
molecular weight, complex heteropolysaccharides may exhibit variations in proportions of sugar
55
constituents, linkage type, or degree and arrangement of branching. In addition, the
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monosaccharide units of some polysaccharides may be sulfated, acetylated, methylated or
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substituted by other groups. Therefore, these polysaccharides may also have difference in the
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degree of substitution.
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Because relatively small differences in molecular weight and structure of polysaccharides
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may result in substantial differences in their physicochemical properties, the availability of
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samples with sufficiently high uniformity constitutes an indispensable requirement in the fields of
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basic research and for analytical purposes (Eckelt, Haase, Loske, & Wolf, 2004). In the former
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case, it is mandatory for the theoretical interpretation of measurements. In the latter, calibration of
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analytical methods often requires high uniformity standards. For instance, size exclusion
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chromatography (SEC) is frequently used for the measurement of molecular weight and molecular
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weight distribution of polymers (Wang, Wood, Huang, & Cui, 2003). Unless the system is
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molecular weight standards have to be used to calibrate the SEC columns. Pullulan and dextran
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are commercially available standards for polysaccharides. However, because the retention volume
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in SEC is dependent on hydrodynamic volume rather than molecular weight, the use of pullulan or
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dextran as standards can lead to inaccurate molecular weight determination of other
72
polysaccharides. On the other hand, some fractions sometimes account for a quite low proportion
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in the polysaccharide sample, so it is difficult to identify these fractions by analyzing the whole
74
polysaccharide sample. Fractionation can enrich these fractions. Therefore, it is necessary to
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fractionate them into more structurally homogeneous materials, particularly for unknown
76
polysaccharides, when examining their molecular structures or structure-property relationships.
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Wide molecular weight distribution of polysaccharides also limits their industrial application. For
78
instance, the molar mass of the hydroxyethyl starch generally used in clinical applications ranges
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40,000~450,000 g/mol and its molar degree of substitution ranges between 0.5 and 0.7 (Gosch,
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Haase, Wolf, & Kulicke, 2002). Hydroxyethyl starch of higher molar mass may induce
81
anaphylactoid reactions. If the hydroxyethyl starch has an excessively low molar mass, it is
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excreted too quickly through the kidneys. There are considerable similar examples. Therefore, it is
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necessary to fractionate polysaccharides into fractions with high homogeneity.
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Fractionation of polysaccharides is mainly performed by chromatography, ultrafiltration and
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gradient non-solvent precipitation. Chromatography and ultrafiltration use columns and
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membranes to fractionate polysaccharides, respectively. Chromatography columns and filtration
87
membranes have their specific molecular weight cut-off, and thus their ranges of application are
88
limited. Fouling of chromatography columns and filtration membranes often result in their short
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industrialization of these two technologies. In addition, these methods are not suitable for
91
large-scale preparations. Fractionation by gradient non-solvent precipitation means that gradual
92
addition of non-solvent into the polysaccharide solution results in gradual precipitation of
93
polysaccharides from the solution. This method is independent of special equipment and only
94
requires simple equipment, such as stirred tanks and centrifuges, making it easily scalable up or
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down according to the need. Therefore, gradient non-solvent precipitation has the most potential
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for preparative fractionation of polysaccharides. In addition, this method has a large scope of
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application for different polysaccharides with different molecular weights. Therefore, fractionation
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of polysaccharides by gradient non-solvent precipitation is reviewed in this work.
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2 The non-solvent
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Usually, the solvent of polysaccharides is water. In an aqueous solution, polysaccharide
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molecules are linked with water molecules by hydrogen bonds, which keep polysaccharides
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soluble in water. The non-solvent can induce the precipitation of polysaccharides from the solution,
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thus the non-solvent is also named as the precipitant. The commonly used precipitants and the
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corresponding polysaccharides are summarized in Table 1. The precipitants include organic
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solvents (methanol, ethanol, isopropanol, acetone and 1-butanol), ammonium sulfate ((NH4)2SO4)
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and polyethylene glycol (PEG).
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Different from other organic solvents, 1-butanol can selectively precipitate amylose due to
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the formation of the amylose-1-butanol complex (Schoch, 1942). Therefore, 1-butanol can be
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exclusively used to fractionate starch into amylose and amylopectin. However, 1-butanol cannot
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fractionate other polysaccharides. Hence, fractionation by 1-butanol is not discussed in this paper.
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agent. These organic solvents have much lower dielectric constant than water. Adding organic
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solvents can lower the dielectric constant of the polysaccharide solution and promote
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intra-molecular associations of water-soluble polysaccharides through competition for water, thus
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inducing conformational changes, aggregation and precipitation of the polysaccharides (Jian, et al.,
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2014). In other words, organic solvents decrease the polarity of water to precipitate
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polysaccharides, because organic solvents have much lower polarity than water (Guo, Meng, Tang,
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et al., 2016). According to the “like dissolves like” principle, the polysaccharides that are initially
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soluble will be eventually precipitated if enough organic solvents are added to decrease the
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polarity of water. The biggest difference of these organic solvents is the dielectric constant (or
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polarity) and their dielectric constant (or polarity) is in the order of methanol > ethanol >
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isopropanol > acetone. Therefore, the precipitation efficiency is in the order of methanol < ethanol
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< isopropanol < acetone. Among these precipitants, ethanol is the most widely used due to its
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safety and food purposes.
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Although the mechanism by which (NH4)2SO4 precipitates polysaccharides is not reported, it
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can be inferred that it is similar to the mechanism by which (NH4)2SO4 precipitates proteins. In an
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aqueous solution, the polysaccharide exposes its polar residues on the surface to maximize the
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contact with water molecules (Huang, et al., 2013). Water molecules bind to the surface of the
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biopolymer and form a hydration layer, which is essential to maintain the solubility and to prevent
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the contact and aggregation of the polysaccharide molecules. The electrostatic repulsion of the
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same charges in the charged polysaccharides also facilitates the interaction between the
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polysaccharides and water. When NH4+ and SO42− ions are added into the aqueous polysaccharide
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hydration layer, facilitating the interactions between the polysaccharide molecules to form
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aggregates and precipitate. In addition, they are attracted to the opposite charges evident on the
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polysaccharide. This attraction of opposite charges also leads to aggregation and precipitation of
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polysaccharides.
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Two chemically different water-soluble polymers are often incompatible in aqueous solutions.
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PEG is incompatible with dextran or dextrin. When the PEG concentration reaches the limiting
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value, phase separation happens and dextran or dextrin is precipitated from the solution. In
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summary, PEG precipitates dextran or dextrin based on their incompatibility. In addition to
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dextran and dextrin, PEG has the potential to fractionally precipitate other polysaccharides, since
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incompatibility widely exists between two chemically different water-soluble polymers. Actually,
144
PEG precipitation has been widely used to purify proteins (Atha & Ingham, 1981;
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Hammerschmidt, Hobiger, & Jungbauer, 2016; Sim, et al., 2012).
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3 The principle of fractionation by gradient non-solvent precipitation
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Fractionation by gradient non-solvent precipitation is based on phase separation of
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polysaccharide solutions. Polysaccharides of different molecular weights or chemical structures
149
have different solubility. Adding small amount of non-solvent initially leads to the precipitation of
150
the polysaccharides with low solubility and subsequent addition of non-solvent gradually
151
precipitates the polysaccharides with relatively high solubility, thereby achieving fractional
152
precipitation of polysaccharides based on differential solubility. Generally, the solubility of
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polysaccharide is negatively correlated to its molecular weight (Hu et al., 2015; Hu, Liu, et al.,
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2017; Hu, Wang, et al., 2017). Therefore, gradient non-solvent precipitation often induces
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addition to the molecular weight, most polysaccharides exhibit variations in proportions of sugar
157
constituents, linkage type, degree and arrangement of branching, and/or degree of substitution,
158
which also result in differential solubility (Izydorczyk & Biliaderis, 1996). Therefore, the mode of
159
fractionation is governed by not only the molecular weight but also the structural characteristics of
160
polysaccharides. Generally, higher precipitant concentration is required to precipitate the
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polysaccharides with the structure characteristics that result in better solubility. For example, when
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galactomannan was fractionated by gradient (NH4)2SO4 precipitation, fractions precipitated at the
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lower saturation level of (NH4)2SO4 had less substituted mannan backbone compared with those
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obtained at a higher salt concentration (Izydorczyk & Biliaderis, 1996). It was also found that the
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less branched hemicelluloses were precipitated at lower ethanol percentages and more branched
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hemicelluloses were obtained at higher ethanol concentrations (Bian et al, 2010). In general,
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depending on the polysaccharide type, various factors, such as high molecular weight, low
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branching levels and high substitution by hydrophobic groups, favor precipitation of
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polysaccharides at low non-solvent concentrations.
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4 Establishment of the fractionation procedure
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Gradient non-solvent precipitation is often carried out as follows (Fig. 2). Non-solvent is
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uniformly added to the polysaccharide solution. Afterward, the solution is held for a certain period
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of time and then centrifuged to obtain the supernatant and precipitate. The residual non-solvent in
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the polysaccharide precipitate should be removed. Organic solvents can be removed by drying.
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After fractionation by (NH4)2SO4, the residual (NH4)2SO4 in the polysaccharide is often removed
176
by dialysis. On the other hand, traces of PEG in the polysaccharide precipitate are often removed
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178
non-solvent into the obtained supernatant, another polysaccharide fraction can be precipitated and
179
be designated as the 2nd fraction. The process of graded precipitation can proceed further to obtain
180
more fractions. The final supernatant is usually abandoned. In theory, the polysaccharides in the
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final supernatant have high dispersity, since different polysaccharide species that are not
182
precipitated are left in the supernatant. In addition, it takes time and energy to remove the
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cumulative non-solvents.
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The stepwise precipitant concentrations used to fractionally precipitate polysaccharides are
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the key of the fractionation procedure. A suitable initial precipitant concentration helps to save
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fractionation time. In order to save time and cost, it is expected to achieve the highest
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polysaccharide yield by using the lowest dose of the precipitant. However, it seems that
188
polysaccharides cannot be completely precipitated from the solution, partially because there are
189
fractions which are soluble at high precipitant concentrations. Therefore, most of the reports try to
190
obtain the best fractionation effect rather than the biggest polysaccharide yield. As is shown in
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Table 2, the final alcohol concentration reached about 80% (v/v) in most cases. Although the
192
alcohol concentration was high, the polysaccharide recovery was often less than 90%. One reason
193
for this result might be that the parent polysaccharides usually contained large amount of
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impurities. However, the ethanol concentration of 33.3% or the isopropanol concentration of
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28.6% resulted in about 90% galactomannan recovery (Jian, et al., 2014). This may be due to the
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fact that galactomannan had very large molecular weight, which was confirmed by the result that
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the galactomannan recovery was positively correlated with the molecular weight. When
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fractionating sugar beet pectin, the highest isopropanol concentration was also very low, about
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beet pectin. Specifically, sugar beet pectin contained high amount of hydrophobic acetyl groups,
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ferulic acids and proteins. In addition, the fractionation procedures in different studies were
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diverse. A previous report that investigated the effect of structural diversity on ethanol
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concentration of precipitating polysaccharide also suggested that the ethanol concentration must
204
be individually optimized for each type of polysaccharide during ethanol precipitation (Xu, et al.,
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2014). Different reports even used different non-solvent concentrations to fractionate the same
206
polysaccharides. Therefore, it is difficult to select non-solvent concentrations for fractionating new
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polysaccharides according to the previous reports. It was suggested that the non-solvent
208
concentrations could be selected based on the curves of the polysaccharide yield as a function of
209
alcohol concentration (Hu, et al., 2015). Hu et al. first precipitated dextrin solutions using different
210
alcohol concentrations to obtain the curves of the dextrin yield as a function of alcohol
211
concentration. According to these curves, the dextrin yield did not significantly increase once the
212
alcohol concentration was 86.7% (v/v). Therefore, fractionation was ended when the alcohol
213
concentration reached 86.7%. When the alcohol concentration was 33.3%, the dextrin yield
214
reached more than 30%. Therefore, the fractionation started from the alcohol concentration at
215
20.0%. On the other hand, Gonzaga et al. added ethanol into the polysaccharide solution until the
216
solution became turbid and stable to obtain the fractions (Gonzaga, et al., 2005). In addition to
217
fractionation, gradient alcohol precipitation can be used to purify polysaccharides. For instance,
218
heparin, dermatan sulfate and chondroitin sulfate in mixtures were successfully separated by
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sequential precipitation with methanol, ethanol or propanol (Volpi, 1996). Similarly, it was found
220
that keratan sulfate could be precipitated prior to chondroitin sulfate (Galeotti, Maccari, & Volpi,
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2014). Therefore, keratan sulfate in chondroitin sulfate samples could be selectively removed by
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sequential precipitation with ethanol. When (NH4)2SO4 is used to fractionate polysaccharides, the (NH4)2SO4 concentration is often
224
characterized by its saturation level. It seemed that (NH4)2SO4 had higher precipitation ability on
225
glucan than other kinds of polysaccharides. Li et al. reported that β-glucans could be precipitated
226
at a much lower saturation level of (NH4)2SO4 than arabinoxylans (Li, et al., 2006). Based on this
227
principle, wheat β-glucan was separated from wheat arabinoxylan by gradient (NH4)2SO4
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precipitation.
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In summary, the precipitation efficiency of organic solvents is the lowest, partially because
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they are liquid. Compared with addition of solid (NH4)2SO4 and PEG, addition of equal organic
231
solvents greatly increases the volume of the polysaccharide solution and decreases the
232
polysaccharide concentration. To fractionate a new polysaccharide, it is suggested to first obtain
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the curve of the polysaccharide recovery as a function of the non-solvent concentration and then
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establish the fractionation procedure according to the curve.
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5 Assessment of the fractionation effect
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Sometimes, fractionation of polysaccharides just helps to enrich fractions and characterize
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polysaccharides. In this case, the fractionation effect is not assessed. Sometimes, the aim of
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fractionation is to obtain fractions with high homogeneity. Afterward, different fractions are used
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for different specific purposes. In this case, the molecular weight homogeneity and structural
240
homogeneity of fractions obtained by fractionation should be determined to assess the
241
fractionation effect. The homogeneity of molecular weight could be indicated by the
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molecular-weight dispersity (DM) (Stepto, 2010). The DM is calculated as the ratio of the
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the polysaccharides is larger than the Mn. Therefore, a lower DM indicates a narrower molecular
245
weight distribution of the polysaccharides. When most of fractions obtained by fractionation have
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smaller DM than the parent polysaccharide, the fractionation is considered to be successful. One
247
sample is always fractionated into several fractions, and different fractionation conditions always
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result in different mass distribution and molecular weight distribution of fractions. Therefore, the
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average molecular-weight dispersity (DMa) was defined as follows to assess the fractionation
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effect:
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DMa =
∑ (X
i
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∑X
i
where DMa was the average dispersity of the fractions in one group, DMi was the dispersity of the
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ith fraction, and the Xi was the mass fraction of the ith fraction (Hu, et al., 2016; Hu, Wang, et al.,
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2017). The lowest DMa indicated the best fractionation effect. However, structural homogeneity,
255
including proportions of sugar constituents, linkage type, degree and arrangement of branching,
256
and the degree of substitution, is difficult to assess and so far no related research is reported.
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6 Factors that affect fractionation
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In theory, fractionation by gradient non-solvent precipitation is affected by the precipitation
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conditions and those factors which affect the solubility of polysaccharides. The molecular weight
260
of polysaccharide affects its solubility, so it also affects fractionation. It was found that the higher
261
the level of high-molecular-weight dextrin, the broader the molecular weight distribution of the
262
different dextrin fractions (Gelders, et al., 2003). Definitely, the effect of the molecular weight and
263
structure of polysaccharides on fractionation cannot be eliminated. Therefore, more effort should
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be made to eliminate the negative effect of the external factors. The external factors are as follows:
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6.1 The rate of adding the precipitant It is easy to understand that the rate of adding the precipitant affects the precipitation process,
267
particularly gradient precipitation during which limited precipitants are used to precipitate the
268
polysaccharides. It was reported that the dextrin yield was higher when alcohol was quickly added
269
than when it was slowly added (Hu, et al., 2015). It was postulated that adding alcohol fast
270
resulted in extremely high alcohol concentration in certain parts of the dextrin solution, thus
271
resulting in co-precipitation of the dextrin. As a result, the rate of adding alcohol should be
272
carefully controlled during fractionation of dextrin by gradient alcohol precipitation. Similar
273
phenomena occur to precipitation by (NH4)2SO4. Therefore, (NH4)2SO4 is often ground into
274
powders. Alternatively, a saturated (NH4)2SO4 solution is used to avoid extremely high (NH4)2SO4
275
concentration in certain parts. Similarly, (NH4)2SO4 powder or solution should be slowly added
276
into
277
PEG-polysaccharide-water system over the phase separation temperature. On the other hand, PEG
278
is not quickly dissolved in water like these organic solvents and (NH4)2SO4. Therefore, combined
279
with heating and stirring, quick addition of PEG is feasible during fractionation by PEG (Hu, et al.,
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2016). Alternatively, a PEG solution may be used in future.
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6.2 The precipitant
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solution.
The
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does
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to
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Due to non-specificity, the three types of precipitants can be widely used to fractionate
283
different kinds of polysaccharides. Basedow & Ebert used ethanol and PEG to fractionate dextran
284
and found that the fractionation results of the two precipitants had no significant difference
285
(Basedow & Ebert, 1979). However, Hu et al. found gradient alcohol precipitation had better
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In addition, the fractionation effect of alcohols was in the order of methanol > ethanol >
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isopropanol, while the precipitation efficiency was in the reverse order (Hu, et al., 2015). With
289
regard to the choice of non-solvent, it should be noted that the non-solvent cannot have very
290
strong precipitation ability (Zhang, et al., 2011). Otherwise, the fractionation will be difficult to
291
control. For example, if one polysaccharide can be completely precipitated by adding ethanol at
292
the concentration of 5% (v/v), it is almost impossible to control such a fractionation process. A
293
suitable non-solvent is the one that can provide a board range of concentration to use. In this case,
294
it is easy to control the fractionation process and adjust the non-solvent concentration for best
295
fractionation. The suitable non-solvent may also be found from the curves of the polysaccharide
296
recovery as a function of the non-solvent concentration.
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6.3 The precipitation temperature
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The precipitation temperature mainly affects the precipitation efficiency. Low fractionation
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temperature decreases the polarity of solvents and solubility of polysaccharides, thus improving
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the precipitation efficiency. Because the precipitation efficiency of organic solvents is relatively
301
low, it is suggested to preform fractionation by gradient organic solvent precipitation at low
302
temperature (Gelders, et al., 2003). Therefore, fractionation by organic solvents is often performed
303
at 4 oC. However, the solubility of (NH4)2SO4 and PEG is low at low temperature and their
304
precipitation efficiency is relatively high at room temperature. Therefore, fractionation by
305
(NH4)2SO4 and PEG is often carried out at room temperature.
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6.4 The precipitation time
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The precipitation time may affect the polysaccharide recovery. It was found that the solubility
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ACCEPTED MANUSCRIPT of polysaccharides in ethanol was so poor that the precipitation of polysaccharides was always
309
quickly finished within minutes (Xu, et al., 2014). Similarly, it was inferred that precipitation of
310
polysaccharides by (NH4)2SO4 was quickly finished. However, after the previous studies usually
311
kept the polysaccharide solution added with organic solvents or (NH4)2SO4 at the precipitation
312
temperature for 1 h or overnight to fully precipitate the polysaccharides. The phase separation of
313
the polymer solution induced by another polymer is very slow. Therefore, the precipitation time of
314
gradient PEG precipitation was 24 h (Hu, et al., 2016; Hu, Wang, et al., 2017).
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6.5 The initial polysaccharide concentration
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As stated above, fractionation by gradient non-solvent precipitation is based on differential
317
solubility of the polysaccharides. The solubility of polysaccharides is dependent on their
318
molecular weight and chemical structure. Undoubtedly, the polysaccharide solubility also depends
319
on its concentration. Therefore, the initial polysaccharide concentration may affect fractionation of
320
polysaccharide. The key of graded precipitation is to avoid co-precipitation of different
321
components. Therefore, the polysaccharide concentration cannot be too high, as co-precipitation
322
easily happens at high concentration, especially in the first fraction. The fractionation result is
323
usually better when the concentration of the polysaccharide solution is lower. But if the
324
polysaccharide concentration is too low, the recovery of polysaccharide will decrease and the
325
consumption of the non-solvent will greatly increase. In general, the initial polysaccharide
326
concentration often ranges from 0.1% to 4% (w/v), which is usually negatively correlated with the
327
molecular weight. However, the most suitable initial concentration may depend on many factors.
328
Hu et al. found that when dextrin was fractionally precipitated by ethanol, the optimal initial
329
concentration was in the range of 1.8%–2.7% (Hu, et al., 2015). However, when fractionating the
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same dextrin by gradient PEG precipitation, the initial dextrin concentration, which ranged from
331
0.9% to 3.6%, did not affect the DMa of the dextrin fractions (Hu, Wang, et al., 2017).
332
6.6 The pH Hydroxyl groups in polysaccharide chain are ionized at high pH (Hedayati, Shahidi,
334
Koocheki, Farahnaky, & Majzoobi, 2016). Alkali can also break the intermolecular hydrogen
335
bonds of polysaccharide. Thus, pH can affect the polysaccharide solubility. In addition, the
336
solubility of charged polysaccharides is more sensitive to pH, because pH can affect the ionization
337
of dissociable groups in charged polysaccharides, such as carboxyl groups and amino groups. It
338
was also reported that pH had a significant effect on the alcoholic precipitation of sugar beet
339
pectin (Guo, Meng, Tang, et al., 2016). Therefore, pH is likely to affect fractionation of
340
polysaccharides. Hu et al. found that neutral environment was the most suitable for fractionation
341
of dextrin by gradient alcohol precipitation, while a weakly alkaline environment was optimal for
342
fractionation of dextrin by gradient PEG precipitation (Hu, Liu, et al., 2017; Hu, Wang, et al.,
343
2017). The pH could change the solubility of dextrin in alcohol or PEG solution. Theoretically, the
344
most suitable pH for dextrin fractionation was the one that could provide the greatest solubility
345
difference between high-molecular-weight dextrin and low-molecular-weight dextrin. Therefore, it
346
was likely that neutral and slightly alkaline environment provided the greatest solubility difference
347
between high-molecular-weight dextrin and low-molecular-weight dextrin in the alcohol and PEG
348
solution, respectively. However, the effect of pH on fractionation of other polysaccharides has not
349
been reported yet. Previous reports often fractionated polysaccharides in a neutral environment.
350
6.7 Other factors
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When alcohol was used as the precipitant, salt also affected fractionation (Hu, Liu, et al.,
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ACCEPTED MANUSCRIPT 2017). When dextrin was fractionated in KCl solutions, salt was co-precipitated with dextrin. KCl
353
resulted in earlier precipitation of dextrin compared to salt-free solution and co-precipitation of
354
dextrin, which was in accordance with the conclusion that salts decreased the solubility of starch
355
(Zhou, et al., 2014). In this case, salt might decrease the solubility difference of dextrin with
356
different sizes, thus negatively affecting fractionation of dextrin. A similar phenomenon may occur
357
to other polysaccharides. In addition, the cation-pectin electrostatic interaction significantly
358
weakened the hydration degree of sugar beet pectin, especially when divalent cations were used,
359
and the combined effect of added counter cations and ethanol led to a significant increase in the
360
precipitation of negatively-charged sugar beet pectin (Guo, Zhang, Meng, & Yu, 2017). Therefore,
361
divalent cations may affect fractionation of pectin and other negatively charged polysaccharides
362
through electrostatic interaction.
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When PEG was used as the precipitant, fractionation was also affected by the molecular
364
weight and molecular weight distribution of PEG (Hu, et al., 2016). PEG with high molecular
365
weight (over 20000 Da) could induce very high viscosity of the solution, which impeded
366
fractionation. Furthermore, fractionation was best accomplished by the most narrowly-distributed
367
PEG.
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7 Conclusions
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Gradient non-solvent precipitation provides a simple and facile way for preparative
370
fractionation of polysaccharides. The non-specificity of the non-solvents makes this method
371
suitable for fractionating almost all kinds of polysaccharides. The fractionation result is affected
372
by various factors and difficult to predict. In theory, enlarging the solubility difference among
373
polysaccharides facilitates fractionation by gradient precipitation. However, the non-specificity of
18
ACCEPTED MANUSCRIPT these precipitants makes it difficult to obtain products with enough uniformity. Therefore, it is still
375
a long-standing challenge to get access to structurally-homogeneous polysaccharides, especially
376
polysaccharides with high molecular weight. Repeated fractionation by one non-solvent or
377
combination of different non-solvents may help to obtain polysaccharides with high uniformity. To
378
extend industrial application of this method, further research is needed to shorten the fractionation
379
time and design special equipment for improving its continuity of operation.
380
Acknowledgements
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This work was supported by the National Natural Science Foundation of China (31601425)
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and Project of Jiangxi Province Education Department (GJJ160187).
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Fig. 1 Schematic representation of fractionating polysaccharides by gradient non-solvent
574
precipitation in the descending order of molecular weight.
575
Fig. 2 The fractionation procedure by gradient non-solvent precipitation.
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Table 1 The commonly used precipitants and the corresponding polysaccharides. Polysaccharide
Reference
Methanol
Dextran
John Eckelt, Sugaya, & Wolf, 2006; Zief, Brunner, & Metzendorf, 1955
Dextrin
Bertoft, 1989; Gelders, Bijnens, Loosveld, Vidts, & Delcour, 2003; Hu, Liu, Jin, & Tian,
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Precipitant
2015
Basedow & Ebert, 1979; Neuchl & Mersmann, 1995, 1996
Dextrin
Defloor , Vandenreyken, Grobet, & Delcour, 1998; Frigard, Andersson, & Aman, 2002;
TE D
Dextran
Gelders, et al., 2003; Hu, Liu, Jin, & Tian, 2017; Hu, et al., 2015
Arabinan
Dervilly, Saulnier, Roger, & Thibault, 2000
EP
Wheat arabinoxylan
AC C
Ethanol
Cardoso, Silva, & Coimbra, 2002
Polysaccharides from Agaricus blazei Murill fructan
Gonzaga, Ricardo, Heatley, & Soares, 2005
Fructan
Paseephol, Small, & Sherkat, 2007; Pourfarzad, Habibi Najafi, Haddad Khodaparast, Hassanzadeh Khayyat, & Malekpour, 2014
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Bian, Peng, Peng, Xu, & Sun, 2010; Li, et al., 2016; Peng, et al., 2009; Peng, et al., 2010;
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Hemicellulose
Peng, et al., 2013; Peng, Peng, Bian, Xu, & Sun, 2011; Shi, Yang, Lin, & Peng, 2013;
SC
Xue, Wen, Xu, & Sun, 2012 Kang, et al., 2011
Exopolysaccharides from Cordyceps sinensis fungus
Huang, Siu, Wang, Cheung, & Wu, 2013
Polysaccharides
Zha, et al., 2012
from
Laminaria
japonica
Jian, et al., 2014
Pectin
Guo, Meng, Zhu, et al., 2016
Lycium
barbarum
AC C
from
Feng, Yin, Nie, Wan, & Xie, 2016
EP
Polysaccharides from Cassia obtusifolia Polysaccharides
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Galactomannan gum
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Gum ghatti
Gong, et al., 2017
Polysaccharides from Moringaoleifera Lam. Leaves
Chen, Zhang, Huang, Fu, & Liu, 2017
Glucan
Wang, et al., 2017
Polysaccharide
form
Polyporus
umbellatus He, et al., 2017
ACCEPTED MANUSCRIPT
Li, Wang, Zheng, & Li, 2017
Dextran
Neuchl & Mersmann, 1996
Dextrin
Gelders, et al., 2003; Hu, et al., 2015
Galactomannan gum
Jian, et al., 2014
Pectin
Karnik, Jung, Hawking, & Wicker, 2016; Karnik & Wicker, 2018; Nagel, et al., 2017
Acetone
Pullulan
John Eckelt, et al., 2006
1-Butanol
Starch
Cornell, McGrane, & Melbourne, 1999; Klucinec & Thompson, 1998; Li & Zhu, 2018;
SC
M AN U
TE D
Isopropanol
RI PT
Polysaccharides from Gynura procumbens
Schoch, 1942 Izydorczyk & Biliaderis, 1992
EP
Arabinoxylan Galactomannan Glucan
AC C
(NH4)2SO4
Mushroom polysaccharides
Izydorczyk, &Biliaderis, 1996 Izydorczyk, Biliaderis, Macri, & MacGregor, 1998; Li, Cui, & Kakuda, 2006; Ragaee, et al., 2008; Wang, et al., 2003 Zhang, et al., 2011
ACCEPTED MANUSCRIPT
Guan, et al., 2015; Peng, et al., 2012
Polysaccharide from leaf skin of Aloe barbadensis
Shi, et al., 2017
RI PT
Hemicellulose
Basedow & Ebert, 1979
Dextrin
Hu, Liu, Jin, & Tian, 2016; Hu, Wang, Liu, Jin, & Tian, 2017
EP
TE D
M AN U
Dextran
AC C
PEG
SC
Miller
ACCEPTED MANUSCRIPT
Non-solvent concentrations
Polysaccharide
Methanol (v/v)
20%, 33%, 50%, 66.7%, 75%, 80% and 83%
Dextrin
Ethanol (v/v)
20%, 33%, 50%, 66.7%, 75%, 80% and 83%
Dextrin
20%, 30%, 40%, 50%, 60% and 70% 50%, 65% and 80%
Reference Hu, et al., 2015 Hu, et al., 2015; Hu, Liu, et al., 2017
Arabinoxylan
Dervilly, et al., 2000
Arabinan
Cardoso, et al., 2002
Hemicellulose
Peng, et al., 2009; Peng, et al., 2010
TE D
15%, 30% and 60%
SC
Non-solvent
M AN U
RI PT
Table 2 Examples of the non-solvent concentrations used during gradient precipitation.
Hemicellulose
Bian, et al., 2010
Hemicellulose
Peng, et al., 2011
Hemicellulose
Xue, et al., 2012
Hemicellulose
Peng, et al., 2013
50%, 67%, 75%, 83% and 88%
Hemicellulose
Shi, et al., 2013
15%, 30%, 45% and 60%
Hemicellulose
Li, et al., 2016
10%, 20%, 30%, 45%, 60% and 80%
EP
15%, 30%, 45%, 60% and 75%
20%, 40%, 60% and 80%
AC C
15%, 60% and 90%
ACCEPTED MANUSCRIPT
17%, 29%, 50%, 67% and 84%
Polysaccharide from Cordyceps sinensis
Huang, et al., 2013
40%, 60% and 80%
Polysaccharide from Laminaria japonica
Zha, et al., 2012
23.1%, 28.6% and 33.3%
Galactomannan gum
Jian, et al., 2014
50%, 67%, 71%, 75%, 78% and 80%
Pectin
Guo, Meng, Zhu, et al., 2016
Polysaccharide from Lycium barbarum
Gong, et al., 2017
Polysaccharide from Moringaoleifera Lam
Chen, et al., 2017
SC
RI PT
Gum ghatti
M AN U
Kang, et al., 2011
50%, 65% and 80%
30%, 50% and 70%
TE D
40%, 60% and 80%
Glucan
Wang, et al., 2017
Polysaccharide from Gynura procumbens
Li, et al., 2017
Dextrin
Hu, et al., 2015
Galactomannan
Jian, et al., 2014
10%, 18%, 25%, 31%, 36% and 40%
Sugar beet pectin
Karnik, et al., 2016
10%, 18%, 25% and 31%
Sugar beet pectin
Karnik & Wicker, 2018
30%, 50% and 70%
EP
20%, 40%, 60% and 80% 20%, 33%, 50%, 66.7%, 75%, 80% and 83%
(v/v)
16.7%, 23.1% and 28.6%
AC C
Isopropanol
ACCEPTED MANUSCRIPT
Arabinoxylan
saturation level
20%, 30%, 45%, 80% and 100%
Galactomannan
70%, 80% and 100%
Galactomannan
30%, 35%, 40% and 50%
Glucan
15%, 15.5%, 16%, 16.3%, 16.6%, 17.2% and 21% 15.5%, 16.7%, 17.8%, 18.3%, 20%, 21.1% and 24%
and 33.5%
PEG
AC C
5%, 15%, 25%, 40%, 55% and 70%
EP
16.4%, 16.8%,17.5%, 18.5%, 19.5%, 23.2%, 28.5%
the initial addition 5 g, stepwise 5 g, the final addition 80 g (For 100 mL solution)
SC
Izydorczyk, &Biliaderis, 1996 Izydorczyk, &Biliaderis, 1996 Izydorczyk, et al., 1998
Glucan
Wang, et al., 2003
Glucan
Wang, et al., 2003
Glucan
Li, et al., 2006
TE D
16.2%, 17.01%, 18.01%, 19.44%, 24% and 40%
RI PT
60%, 70%, 80% and 95%
M AN U
Izydorczyk & Biliaderis, 1992
(NH4)2SO4
Glucan
Ragaee, et al., 2008
Polysaccharide from Aloe barbadensis Miller
Guan, et al., 2015
Dextrin
Hu, et al., 2016; Hu, Wang, et al., 2017
ACCEPTED MANUSCRIPT Fig. 1 Schematic representation of fractionating polysaccharides by gradient non-solvent
AC C
EP
TE D
M AN U
SC
RI PT
precipitation in the descending order of molecular weight.
ACCEPTED MANUSCRIPT
AC C
EP
TE D
M AN U
SC
RI PT
Fig. 2 The fractionation procedure by gradient non-solvent precipitation.
ACCEPTED MANUSCRIPT Gradient precipitation is based on solubility differences of polysaccharides. Polysaccharides are generally precipitated in descending order of molecular weight. Non-solvents of polysaccharides mainly include organic solvents, (NH4)2SO4 and PEG.
AC C
EP
TE D
M AN U
SC
RI PT
Fractionation of polysaccharides by this method is affected by various factors.
1