38482-82-5

Basic information

• Product Name: R,S Equol 7--D-Glucuronide
• Synonyms: 3,4-Dihydro-3-(4-hydroxyphenyl)-2H-1-benzopyran-7-yl--D-glucopyranosiduronic Acid;Equol Glucuronide;R,S Equol 7--D-Glucuronide;Equol 7-glucuronide;(3S)-3,4-Dihydro-3-(4-hydroxyphenyl)-2H-1-benzopyran-7-yl beta-D-glucopyranosiduronic acid
• CAS NO: 38482-82-5
• Molecular Formula: C21H22O9
• Molecular Weight: 418.39398
• Product Categories: Glucuronides;Metabolites & Impurities
• Mol File: 38482-82-5.mol
• Article Data: 1

Chemical Properties

• Melting Point: 140-142°C
• Appearance: /
• Storage Temp.: Hygroscopic, -20?C Freezer, Under Inert Atmosphere
• CAS DataBase Reference: R,S Equol 7--D-Glucuronide(CAS DataBase Reference)
• NIST Chemistry Reference: R,S Equol 7--D-Glucuronide(38482-82-5)
• EPA Substance Registry System: R,S Equol 7--D-Glucuronide(38482-82-5)

Safety Data

• Hazardous Substances Data: 38482-82-5(Hazardous Substances Data)

Usage

Description

R,S Equol 7--D-Glucuronide is a glucuronide metabolite of isoflavone Daidzein, a type of isoflavone found in soybeans and other legumes. It is formed through the process of glucuronidation, which is a metabolic pathway that helps the body to eliminate waste products and toxins.

Uses

Used in Pharmaceutical Industry:
R,S Equol 7--D-Glucuronide is used as a pharmaceutical agent for its potential health benefits. It has been studied for its potential to improve cardiovascular health, reduce the risk of certain types of cancer, and alleviate menopausal symptoms.
Used in Nutraceutical Industry:
R,S Equol 7--D-Glucuronide is used as a nutraceutical ingredient in dietary supplements and functional foods. It is believed to have antioxidant properties and may help to support overall health and well-being.
Used in Research:
R,S Equol 7--D-Glucuronide is used as a research compound to study the metabolism and health effects of isoflavones. It can help scientists to better understand the mechanisms by which isoflavones exert their health benefits and to develop new therapies and interventions based on this knowledge.

Upstream product

• 1245697-26-0 UDP-glucuronic acid 
• 531-95-3 equol 

Relevant articles and documents

Accurate prediction of glucuronidation of structurally diverse phenolics by human UGT1A9 using combined experimental and in silico approaches

Purpose: Catalytic selectivity of human UGT1A9, an important membrane-bound enzyme catalyzing glucuronidation of xenobiotics, was determined experimentally using 145 phenolics and analyzed by 3D-QSAR methods. Methods: Catalytic efficiency of UGT1A9 was determined by kinetic profiling. Quantitative structure activity relationships were analyzed using CoMFA and CoMSIA techniques. Molecular alignment of substrate structures was made by superimposing the glucuronidation site and its adjacent aromatic ring to achieve maximal steric overlap. For a substrate with multiple active glucuronidation sites, each site was considered a separate substrate. Results: 3D-QSAR analyses produced statistically reliable models with good predictive power (CoMFA: q 2=0.548, r2=0.949, r pred 2 =0.775; CoMSIA: q2=0.579, r2=0.876, rpred2 =0.700). Contour coefficient maps were applied to elucidate structural features among substrates that are responsible for selectivity differences. Contour coefficient maps were overlaid in the catalytic pocket of a homology model of UGT1A9, enabling identification of the UGT1A9 catalytic pocket with a high degree of confidence. Conclusion: CoMFA/CoMSIA models can predict substrate selectivity and in vitro clearance of UGT1A9. Our findings also provide a possible molecular basis for understanding UGT1A9 functions and substrate selectivity.