Literature DB >> 24100038

The inhibitory effects of a rhamnogalacturonan I (RG-I) domain from ginseng pectin on galectin-3 and its structure-activity relationship.

Xiaoge Gao1, Yuan Zhi1, Lin Sun1, Xiaoxia Peng1, Tao Zhang1, Huiting Xue1, Guihua Tai2, Yifa Zhou3.   

Abstract

Pectin has been shown to inhibit the actions of galectin-3, a β-galactoside-binding protein associated with cancer progression. The structural features of pectin involved in this activity remain unclear. We investigated the effects of different ginseng pectins on galectin-3 action. The rhamnogalacturonan I-rich pectin fragment, RG-I-4, potently inhibited galectin-3-mediated hemagglutination, cancer cell adhesion and homotypic aggregation, and binding of galectin-3 to T-cells. RG-I-4 specifically bound to the carbohydrate recognition domain of galectin-3 with a dissociation constant of 22.2 nm, which was determined by surface plasmon resonance analysis. The structure-activity relationship of RG-I-4 was investigated by modifying the structure through various enzymatic and chemical methods followed by activity tests. The results showed that (a) galactan side chains were essential to the activity of RG-I-4, whereas arabinan side chains positively or negatively regulated the activity depending on their location within the RG-I-4 molecule. (b) The activity of galactan chain was proportional to its length up to 4 Gal residues and largely unchanged thereafter. (c) The majority of galactan side chains in RG-I-4 were short with low activities. (d) The high activity of RG-I-4 resulted from the cooperative action of these side chains. (e) The backbone of the molecule was very important to RG-I-4 activity, possibly by maintaining a structural conformation of the whole molecule. (f) The isolated backbone could bind galectin-3, which was insensitive to lactose treatment. The novel discovery that the side chains and backbone play distinct roles in regulating RG-I-4 activity is valuable for producing highly active pectin-based galectin-3 inhibitors.

Entities:  

Keywords:  Carbohydrate Structure; Carbohydrate-binding Protein; Galectin; Galectin-3 Inhibitors; Ginseng Pectin; Oligosaccharide; Polysaccharide; Rhamnogalacturonan I; Structure-Activity Relationship

Mesh:

Substances:

Year:  2013        PMID: 24100038      PMCID: PMC3837135          DOI: 10.1074/jbc.M113.482315

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  40 in total

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2.  Synthesis of galactose-mimicking 1H-(1,2,3-triazol-1-yl)-mannosides as selective galectin-3 and 9N inhibitors.

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Journal:  Carbohydr Res       Date:  2007-03-14       Impact factor: 2.104

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5.  Recognition of galactan components of pectin by galectin-3.

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Journal:  Carbohydr Res       Date:  2008-09-26       Impact factor: 2.104

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Journal:  Drug Resist Updat       Date:  2007-06-04       Impact factor: 18.500

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2.  Homogalacturonan from squash: Characterization and tau-binding pattern of a sulfated derivative.

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3.  Novel polysaccharide binding to the N-terminal tail of galectin-3 is likely modulated by proline isomerization.

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Journal:  Glycobiology       Date:  2017-11-01       Impact factor: 4.313

4.  Galectin-3 N-terminal tail prolines modulate cell activity and glycan-mediated oligomerization/phase separation.

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5.  Crystallization of Galectin-8 Linker Reveals Intricate Relationship between the N-terminal Tail and the Linker.

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6.  Nanocoating with plant-derived pectins activates osteoblast response in vitro.

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7.  Plant-derived pectin nanocoatings to prevent inflammatory cellular response of osteoblasts following Porphyromonas gingivalis infection.

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Review 8.  Ginseng and anticancer drug combination to improve cancer chemotherapy: a critical review.

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9.  Low or No Inhibitory Potency of the Canonical Galectin Carbohydrate-binding Site by Pectins and Galactomannans.

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Journal:  J Biol Chem       Date:  2016-04-26       Impact factor: 5.157

Review 10.  Galectin-3 Activation and Inhibition in Heart Failure and Cardiovascular Disease: An Update.

Authors:  Navin Suthahar; Wouter C Meijers; Herman H W Silljé; Jennifer E Ho; Fu-Tong Liu; Rudolf A de Boer
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