期刊
REDOX BIOLOGY
卷 58, 期 -, 页码 -出版社
ELSEVIER
DOI: 10.1016/j.redox.2022.102540
关键词
GTP cyclohydrolase 1; S-nitrosylation; Endothelial cell; Vascular cognitive impairment; Nitrosative stress
资金
- National Key R&D Program of China [2020YFC2008000, 2020YFC2008004]
- National Natural Science Foundations of China [82271460, 82270388, 81970693, U1804197, 81874312, 81770493]
- National High-End Foreign Expert Recruitment Plan of China [G2022026006L]
- Research Foundation of Henan Province [202300410308, HNGD2022067, 212102311046]
- Natural Science Foundations of Shandong Province [2019GSF108070]
- Zhong-Yuan-Qian-Ren Program of Henan province [194200510005]
- Tai-Hang Professional Scholarship of Xinxiang Medical University [505067]
This study demonstrates that HHcy induces GCH1 protein S-nitrosylation, leading to cerebral vascular stiffness and cognitive impairments.
Background: s: Hyperhomocysteinemia (HHcy) is one of risk factors for vascular cognitive impairment (VCI). GTP cyclohydrolase 1 (GCH1) deficiency is critical to oxidative stress in vascular dysfunction. The aim of this study was designed to examine whether HHcy induces VCI through GCH1 S-nitrosylation, a redox-related post-translational modification of cysteine.Methods: The VCI model was induced by feeding mice homocysteine thiolactone (HTL) for 16 consecutive weeks. The cognitive functions were evaluated by step-down avoidance test, passive avoidance step-through task test, and Morris water maze (MWM) test. Protein S-nitrosylation was assayed using a biotin-switch method.Results: In cell-free system, nitric oxide (NO) donor induced GCH1 protein S-nitrosylation and decreased GCH1 activity. In endothelial cells, HTL increased GCH1 S-nitrosylation, reduced tetrahydrobiopterin, and induced oxidative stress, which were attenuated by N-acetyl-cysteine, L-N6-1-Iminoethyl-lysine, mutant of GCH1 cysteine 141 to alanine (MT-GCH1) or gene deletion of inducible NO synthase (iNOS). Further, HTL incubation or iNOS overexpression promoted endothelial cellular senescence, but abolished by exogenous expression of MT-GCH1 or pharmacological approaches including N-acetyl-cysteine, L-sepiapterin, and tempol. In wildtype mice, long-term administration of HTL induced GCH1 S-nitrosylation and vascular stiffness, decreased cerebral blood flow, and damaged the cognitive functions. However, these abnormalities induced by HTL administration were rescued by enforced expression of MT-GCH1 or gene knockout of iNOS. In human subjects, GCH1 S-nitrosylation was increased and cognitive functions were impaired in patients with HHcy.Conclusion: The iNOS-mediated nitrosative stress induced by HTL drives GCH1 S-nitrosylation to induce cerebral vascular stiffness and cognitive impairments.
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