Literature DB >> 31170387

Inhibition of human carboxylesterases by magnolol: Kinetic analyses and mechanism.

Yun-Qing Song1, Zi-Miao Weng2, Tong-Yi Dou3, Moshe Finel4, Ya-Qiao Wang1, Le-Le Ding1, Qiang Jin1, Dan-Dan Wang1, Sheng-Quan Fang1, Yun-Feng Cao5, Jie Hou6, Guang-Bo Ge7.   

Abstract

Magnolol, the most abundant bioactive constituent of the Chinese herb Magnolia officinalis, has been found with multiple biological activities, including anti-oxidative, anti-inflammatory and enzyme-regulatory activities. In this study, the inhibitory effects and inhibition mechanism of magnolol on human carboxylesterases (hCEs), the key enzymes responsible for the hydrolytic metabolism of a variety of endogenous esters as well as ester-bearing drugs, have been well-investigated. The results demonstrate that magnolol strongly inhibits hCE1-mediated hydrolysis of various substrates, whereas the inhibition of hCE2 by magnolol is substrate-dependent, ranging from strong to moderate. Inhibition of intracellular hCE1 and hCE2 by magnolol was also investigated in living HepG2 cells, and the results showed that magnolol could strongly inhibit intracellular hCE1, while the inhibition of intracellular hCE2 was weak. Inhibition kinetic analyses and docking simulations revealed that magnolol inhibited both hCE1 and hCE2 in a mixed manner, which could be partially attributed to its binding at two distinct ligand-binding sites in each carboxylesterase, including the catalytic cavity and the regulatory domain. In addition, the potential risk of the metabolic interactions of magnolol via hCE1 inhibition was predicted on the basis of a series of available pharmacokinetic data and the inhibition constants. All these findings are very helpful in deciphering the metabolic interactions between magnolol and hCEs, and also very useful for avoiding deleterious interactions via inhibition of hCEs.
Copyright © 2019 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  Herb-drug interactions (HDIs); Human carboxylesterases (hCEs); Inhibition potential; Magnolol

Mesh:

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Year:  2019        PMID: 31170387     DOI: 10.1016/j.cbi.2019.06.003

Source DB:  PubMed          Journal:  Chem Biol Interact        ISSN: 0009-2797            Impact factor:   5.192


  6 in total

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2.  Rapalogues as hCES2A Inhibitors: In Vitro and In Silico Investigations.

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4.  Inhibition of human thrombin by the constituents of licorice: inhibition kinetics and mechanistic insights through in vitro and in silico studies.

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Journal:  RSC Adv       Date:  2020-01-22       Impact factor: 4.036

5.  Inhibition of human carboxylesterases by ginsenosides: structure-activity relationships and inhibitory mechanism.

Authors:  Zhao-Hui Sun; Jing Chen; Yun-Qing Song; Tong-Yi Dou; Li-Wei Zou; Da-Cheng Hao; Hai-Bin Liu; Guang-Bo Ge; Ling Yang
Journal:  Chin Med       Date:  2019-12-16       Impact factor: 5.455

6.  Inhibition of drug-metabolizing enzymes by Jingyin granules: implications of herb-drug interactions in antiviral therapy.

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Journal:  Acta Pharmacol Sin       Date:  2021-06-28       Impact factor: 6.150

  6 in total

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