Inhibition of human carboxylesterases by ginsenosides: structure–activity relationships and inhibitory mechanism

Inhibition of human carboxylesterases by ginsenosides: structure–activity relationships and inhibitory mechanism

Abstract Background Human carboxylesterases (hCES) are key serine hydrolases responsible for the hydrolysis of a wide range of endogenous and xenobiotic esters. Although it has been reported that some ginsenosides can modulate the activities of various enzymes, the inhibitory effects of ginsenosides...

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Main 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
Format: Article
Language:English
Published: BMC 2019-12-01
Series:Chinese Medicine
Subjects:
Ginsenosides
Human carboxylesterases (hCES)
Structure–inhibition relationships
Selectivity
Inhibitory mechanism
Online Access:https://doi.org/10.1186/s13020-019-0279-0
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spelling doaj-4d3667e289db486d9e846e2651a677dd2020-12-20T12:21:04ZengBMCChinese Medicine1749-85462019-12-0114111510.1186/s13020-019-0279-0Inhibition of human carboxylesterases by ginsenosides: structure–activity relationships and inhibitory mechanismZhao-Hui Sun0Jing Chen1Yun-Qing Song2Tong-Yi Dou3Li-Wei Zou4Da-Cheng Hao5Hai-Bin Liu6Guang-Bo Ge7Ling Yang8Institute of Interdisciplinary Integrative Medicine Research, Shanghai University of Traditional Chinese MedicineSchool of Life Science and Medicine, Dalian University of TechnologyInstitute of Interdisciplinary Integrative Medicine Research, Shanghai University of Traditional Chinese MedicineSchool of Life Science and Medicine, Dalian University of TechnologyInstitute of Interdisciplinary Integrative Medicine Research, Shanghai University of Traditional Chinese MedicineSchool of Environment and Chemical Engineering, Dalian Jiaotong UniversityNational Engineering Research Center for Gelatin-based Traditional Chinese Medicine, Dong-E-E-Jiao Co. Ltd.Institute of Interdisciplinary Integrative Medicine Research, Shanghai University of Traditional Chinese MedicineInstitute of Interdisciplinary Integrative Medicine Research, Shanghai University of Traditional Chinese MedicineAbstract Background Human carboxylesterases (hCES) are key serine hydrolases responsible for the hydrolysis of a wide range of endogenous and xenobiotic esters. Although it has been reported that some ginsenosides can modulate the activities of various enzymes, the inhibitory effects of ginsenosides on hCES have not been well-investigated. Methods In this study, more than 20 ginsenosides were collected and their inhibitory effects on hCES1A and hCES2A were assayed using the highly specific fluorescent probe substrates for each isoenzyme. Molecular docking simulations were also performed to investigate the interactions between ginsenosides and hCES. Results Among all tested ginsenosides, Dammarenediol II (DM) and 20S-O-β-(d-glucosyl)-dammarenediol II (DMG) displayed potent inhibition against both hCES1A and hCES2A, while protopanaxadiol (PPD) and protopanaxatriol (PPT) exhibited strong inhibition on hCES2A and high selectivity over hCES1A. Introduction of O-glycosyl groups at the core skeleton decreased hCES inhibition activity, while the hydroxyl groups at different sites might also effect hCES inhibition. Inhibition kinetic analyses demonstrated that DM and DMG functioned as competitive inhibitors against hCES1A-mediated d-luciferin methyl ester (DME) hydrolysis. In contrast, DM, DMG, PPD and PPT inhibit hCES2A-mediated fluorescein diacetate (FD) hydrolysis via a mixed manner. Conclusion The structure–inhibition relationships of ginsenosides as hCES inhibitors was investigated for the first time. Our results revealed that DM and DMG were potent inhibitors against both hCES1A and hCES2A, while PPD and PPT were selective and strong inhibitors against hCES2A.https://doi.org/10.1186/s13020-019-0279-0GinsenosidesHuman carboxylesterases (hCES)Structure–inhibition relationshipsSelectivityInhibitory mechanism
collection DOAJ
language English
format Article
sources DOAJ
author 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
spellingShingle 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
Inhibition of human carboxylesterases by ginsenosides: structure–activity relationships and inhibitory mechanism
Chinese Medicine
Ginsenosides
Human carboxylesterases (hCES)
Structure–inhibition relationships
Selectivity
Inhibitory mechanism
author_facet 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
author_sort Zhao-Hui Sun
title Inhibition of human carboxylesterases by ginsenosides: structure–activity relationships and inhibitory mechanism
title_short Inhibition of human carboxylesterases by ginsenosides: structure–activity relationships and inhibitory mechanism
title_full Inhibition of human carboxylesterases by ginsenosides: structure–activity relationships and inhibitory mechanism
title_fullStr Inhibition of human carboxylesterases by ginsenosides: structure–activity relationships and inhibitory mechanism
title_full_unstemmed Inhibition of human carboxylesterases by ginsenosides: structure–activity relationships and inhibitory mechanism
title_sort inhibition of human carboxylesterases by ginsenosides: structure–activity relationships and inhibitory mechanism
publisher BMC
series Chinese Medicine
issn 1749-8546
publishDate 2019-12-01
description Abstract Background Human carboxylesterases (hCES) are key serine hydrolases responsible for the hydrolysis of a wide range of endogenous and xenobiotic esters. Although it has been reported that some ginsenosides can modulate the activities of various enzymes, the inhibitory effects of ginsenosides on hCES have not been well-investigated. Methods In this study, more than 20 ginsenosides were collected and their inhibitory effects on hCES1A and hCES2A were assayed using the highly specific fluorescent probe substrates for each isoenzyme. Molecular docking simulations were also performed to investigate the interactions between ginsenosides and hCES. Results Among all tested ginsenosides, Dammarenediol II (DM) and 20S-O-β-(d-glucosyl)-dammarenediol II (DMG) displayed potent inhibition against both hCES1A and hCES2A, while protopanaxadiol (PPD) and protopanaxatriol (PPT) exhibited strong inhibition on hCES2A and high selectivity over hCES1A. Introduction of O-glycosyl groups at the core skeleton decreased hCES inhibition activity, while the hydroxyl groups at different sites might also effect hCES inhibition. Inhibition kinetic analyses demonstrated that DM and DMG functioned as competitive inhibitors against hCES1A-mediated d-luciferin methyl ester (DME) hydrolysis. In contrast, DM, DMG, PPD and PPT inhibit hCES2A-mediated fluorescein diacetate (FD) hydrolysis via a mixed manner. Conclusion The structure–inhibition relationships of ginsenosides as hCES inhibitors was investigated for the first time. Our results revealed that DM and DMG were potent inhibitors against both hCES1A and hCES2A, while PPD and PPT were selective and strong inhibitors against hCES2A.
topic Ginsenosides
Human carboxylesterases (hCES)
Structure–inhibition relationships
Selectivity
Inhibitory mechanism
url https://doi.org/10.1186/s13020-019-0279-0
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