Hydrogen sulfide lowers hyperhomocysteinemia dependent on cystathionine γ lyase S‐sulfhydration in ApoE‐knockout atherosclerotic mice

BACKGROUND AND PURPOSE: Hydrogen sulfide donors can block the cardiovascular injury of hyperhomocysteinemia. H(2)S also lowers serum homocysteine in rats with mild hyperhomocysteinemia, but the pharmacological mechanism is unknown. The present study investigated the mechanism(s) involved. EXPERIMENT...

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Autores principales: Fan, Jinhui, Zheng, Fengjiao, Li, Shuangyue, Cui, Cangting, Jiang, Shan, Zhang, Jun, Cai, Jun, Cui, Qinghua, Yang, Jichun, Tang, Xinjing, Xu, Guoheng, Geng, Bin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
Materias:
Research Papers
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6692586/
https://www.ncbi.nlm.nih.gov/pubmed/31140595
http://dx.doi.org/10.1111/bph.14719
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author Fan, Jinhui
Zheng, Fengjiao
Li, Shuangyue
Cui, Cangting
Jiang, Shan
Zhang, Jun
Cai, Jun
Cui, Qinghua
Yang, Jichun
Tang, Xinjing
Xu, Guoheng
Geng, Bin
author_facet Fan, Jinhui
Zheng, Fengjiao
Li, Shuangyue
Cui, Cangting
Jiang, Shan
Zhang, Jun
Cai, Jun
Cui, Qinghua
Yang, Jichun
Tang, Xinjing
Xu, Guoheng
Geng, Bin
author_sort Fan, Jinhui
collection PubMed
description BACKGROUND AND PURPOSE: Hydrogen sulfide donors can block the cardiovascular injury of hyperhomocysteinemia. H(2)S also lowers serum homocysteine in rats with mild hyperhomocysteinemia, but the pharmacological mechanism is unknown. The present study investigated the mechanism(s) involved. EXPERIMENTAL APPROACH: ApoE‐knockout mice were fed a Paigen diet and L‐methionine in drinking water for 16 weeks to create a mouse model of atherosclerosis with hyperhomocysteinemia. H(2)S donors (NaHS and GYY4137) were administered by intraperitoneal injection. We also assayed the H(2)S produced (by methylene blue assay and mito‐HS [H(2)S fluorescence probe]), cystathionine γ lyase (CSE) mRNA and protein expression, and CSE sulfhydration and nitrosylation and its activity. KEY RESULTS: H(2)S donor treatment significantly lowered atherosclerotic plaque area, macrophage infiltration, and serum homocysteine level in the mouse model of atherosclerosis with co‐existing hyperhomocysteinemia. mRNA and protein levels of CSE, a key enzyme catalyzing homocysteine trans‐sulfuration, were down‐regulated with hyperhomocysteinemia, and CSE catalytic activity was inhibited. All these effects were reversed with H(2)S donor treatment. Hyperhomocysteinemia induced CSE nitrosylation, whereas H(2)S sulfhydrated CSE at the same cysteine residues. Nitrosylated CSE decreased and sulfhydrated CSE increased its catalytic and binding activities towards L‐homocysteine. Mutation of C252, C255, C307, and C310 residues in CSE abolished CSE nitrosylation or sulfhydration and prevented its binding to L‐homocysteine. CONCLUSIONS AND IMPLICATIONS: Sulfhydration or nitrosylation of CSE represents a yin/yang regulation of catalysis or binding to L‐homocysteine. H(2)S donor treatment enhanced CSE sulfhydration, thus lowering serum L‐homocysteine, which contributed in part to the anti‐atherosclerosis effects in ApoE‐knockout mice with hyperhomocysteinemia.
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spelling pubmed-66925862019-08-19 Hydrogen sulfide lowers hyperhomocysteinemia dependent on cystathionine γ lyase S‐sulfhydration in ApoE‐knockout atherosclerotic mice Fan, Jinhui Zheng, Fengjiao Li, Shuangyue Cui, Cangting Jiang, Shan Zhang, Jun Cai, Jun Cui, Qinghua Yang, Jichun Tang, Xinjing Xu, Guoheng Geng, Bin Br J Pharmacol Research Papers BACKGROUND AND PURPOSE: Hydrogen sulfide donors can block the cardiovascular injury of hyperhomocysteinemia. H(2)S also lowers serum homocysteine in rats with mild hyperhomocysteinemia, but the pharmacological mechanism is unknown. The present study investigated the mechanism(s) involved. EXPERIMENTAL APPROACH: ApoE‐knockout mice were fed a Paigen diet and L‐methionine in drinking water for 16 weeks to create a mouse model of atherosclerosis with hyperhomocysteinemia. H(2)S donors (NaHS and GYY4137) were administered by intraperitoneal injection. We also assayed the H(2)S produced (by methylene blue assay and mito‐HS [H(2)S fluorescence probe]), cystathionine γ lyase (CSE) mRNA and protein expression, and CSE sulfhydration and nitrosylation and its activity. KEY RESULTS: H(2)S donor treatment significantly lowered atherosclerotic plaque area, macrophage infiltration, and serum homocysteine level in the mouse model of atherosclerosis with co‐existing hyperhomocysteinemia. mRNA and protein levels of CSE, a key enzyme catalyzing homocysteine trans‐sulfuration, were down‐regulated with hyperhomocysteinemia, and CSE catalytic activity was inhibited. All these effects were reversed with H(2)S donor treatment. Hyperhomocysteinemia induced CSE nitrosylation, whereas H(2)S sulfhydrated CSE at the same cysteine residues. Nitrosylated CSE decreased and sulfhydrated CSE increased its catalytic and binding activities towards L‐homocysteine. Mutation of C252, C255, C307, and C310 residues in CSE abolished CSE nitrosylation or sulfhydration and prevented its binding to L‐homocysteine. CONCLUSIONS AND IMPLICATIONS: Sulfhydration or nitrosylation of CSE represents a yin/yang regulation of catalysis or binding to L‐homocysteine. H(2)S donor treatment enhanced CSE sulfhydration, thus lowering serum L‐homocysteine, which contributed in part to the anti‐atherosclerosis effects in ApoE‐knockout mice with hyperhomocysteinemia. John Wiley and Sons Inc. 2019-07-14 2019-09 /pmc/articles/PMC6692586/ /pubmed/31140595 http://dx.doi.org/10.1111/bph.14719 Text en © 2019 The Authors. British Journal of Pharmacology published by John Wiley & Sons Ltd on behalf of British Pharmacological Society. This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc-nd/4.0/ License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Research Papers
Fan, Jinhui
Zheng, Fengjiao
Li, Shuangyue
Cui, Cangting
Jiang, Shan
Zhang, Jun
Cai, Jun
Cui, Qinghua
Yang, Jichun
Tang, Xinjing
Xu, Guoheng
Geng, Bin
Hydrogen sulfide lowers hyperhomocysteinemia dependent on cystathionine γ lyase S‐sulfhydration in ApoE‐knockout atherosclerotic mice
title Hydrogen sulfide lowers hyperhomocysteinemia dependent on cystathionine γ lyase S‐sulfhydration in ApoE‐knockout atherosclerotic mice
title_full Hydrogen sulfide lowers hyperhomocysteinemia dependent on cystathionine γ lyase S‐sulfhydration in ApoE‐knockout atherosclerotic mice
title_fullStr Hydrogen sulfide lowers hyperhomocysteinemia dependent on cystathionine γ lyase S‐sulfhydration in ApoE‐knockout atherosclerotic mice
title_full_unstemmed Hydrogen sulfide lowers hyperhomocysteinemia dependent on cystathionine γ lyase S‐sulfhydration in ApoE‐knockout atherosclerotic mice
title_short Hydrogen sulfide lowers hyperhomocysteinemia dependent on cystathionine γ lyase S‐sulfhydration in ApoE‐knockout atherosclerotic mice
title_sort hydrogen sulfide lowers hyperhomocysteinemia dependent on cystathionine γ lyase s‐sulfhydration in apoe‐knockout atherosclerotic mice
topic Research Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6692586/
https://www.ncbi.nlm.nih.gov/pubmed/31140595
http://dx.doi.org/10.1111/bph.14719
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