Structure-activity relationship of synthesized glucans from Ganoderma lucidum with in vitro hypoglycemic activity.

Int J Biol Macromol

State Key Laboratory of Phytochemistry and Plant Resources in West China, Yunnan Key Laboratory of Natural Medicinal Chemistry, Kunming Institute of Botany, Chinese Academy of Sciences, Kunming, Yunnan 650201, China. Electronic address:

Published: December 2024

AI Article Synopsis

  • Synthetic polysaccharides can be utilized to design new drugs by examining their structure-activity relationships (SAR), particularly in terms of protein stability.
  • The study focuses on the glucan GLSWA-1 and its substructures, revealing that compound 2 enhances insulin secretion in a dose-dependent manner while maintaining insulin's thermal stability.
  • Molecular dynamics simulations indicate that compound 2 forms a "groove-binding model" with insulin, suggesting its potential as a hypoglycemic agent due to its favorable structural characteristics.

Article Abstract

The synthetic polysaccharides, which have precise structure, can be used to design new drugs by comparing structure-activity relationships (SAR). Improved protein stability may be due to the interaction between the polysaccharides and protein, which includes covalent and noncovalent interactions. It is critical to investigate the SAR of polysaccharides with a precise structure from the perspective of protein stability. Glucans-insulin interaction may be a useful stratagy to solve this problem. This study reports the SAR of the synthesized glucan GLSWA-1 and its substructures 2-4 on insulin secretion and discusses its mechanism. The results showed that although GLSWA-1 and its substructures 2-4 bind insulin to varying degrees, compound 2 improves insulin secretion in a dose-dependent manner. Further research found that compound 2 maintains the thermal stability of insulin better than GLSWA-1 through stronger hydrogen bonding, and molecular dynamics simulations demonstrated that compound 2 can form a "groove-binding model" with insulin. This study considerably improves the research on the SAR of glucan based on insulin thermostability and indicates that compound 2, its linear structure, appropriate chain flexibility ((1 → 6)-glucoside bonds), low molecular weight, and smaller steric hindrance is a potential hypoglycemic agent.

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Source
http://dx.doi.org/10.1016/j.ijbiomac.2024.138586DOI Listing

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