Gut microbial co-metabolite 2-methylbutyrylcarnitine exacerbates thrombosis via binding to and activating integrin α2β1

代谢物 血小板 血小板活化 整合素 化学 血栓 血栓形成 免疫学 药理学 生物化学 生物 医学 受体 内科学
作者
Kan Huang,Zilun Li,Xi He,Jun Dai,Bingding Huang,Yongxia Shi,Dongxiao Fan,Zefeng Zhang,Yunchong Liu,Na Li,Zhongyu Zhang,Jiangyun Peng,Chenshu Liu,Renli Zeng,Zhipeng Cen,Tengyao Wang,Wenxuan Yang,Meifeng Cen,Jingyu Li,Shuai Yuan,Zhigang Lu,Dandan Hu,Shuxiang Huang,Pin Chen,Peilong Lai,Lih-Yuan Lin,Jielu Wen,Zengxiu Zhao,Xin Huang,Lining Yuan,Lifang Zhou,Haoliang Wu,Lihua Huang,Kai Feng,Jian Wang,Baolin Liao,Wei Cai,Xianwen Deng,Yueping Liu,Jianping Li,Zhongwei Huang,Yang Li,Jiaojiao Li,Youguang Zhuo,Fuchun Zhang,Lin Lin,Yumin Luo,Wei Zhang,Qianlin Ni,Xiqiang Hong,Guangqi Chang,Yaoxin Zhang,Dongxian Guan,Wenju Cai,Yutong Lu,Fang Li,Yan Li,Mindong Ren,Linghua Li,Si-Fan Chen
出处
期刊:Cell Metabolism [Elsevier]
卷期号:36 (3): 598-616.e9 被引量:1
标识
DOI:10.1016/j.cmet.2024.01.014
摘要

Thrombosis represents the leading cause of death and disability upon major adverse cardiovascular events (MACEs). Numerous pathological conditions such as COVID-19 and metabolic disorders can lead to a heightened thrombotic risk; however, the underlying mechanisms remain poorly understood. Our study illustrates that 2-methylbutyrylcarnitine (2MBC), a branched-chain acylcarnitine, is accumulated in patients with COVID-19 and in patients with MACEs. 2MBC enhances platelet hyperreactivity and thrombus formation in mice. Mechanistically, 2MBC binds to integrin α2β1 in platelets, potentiating cytosolic phospholipase A2 (cPLA2) activation and platelet hyperresponsiveness. Genetic depletion or pharmacological inhibition of integrin α2β1 largely reverses the pro-thrombotic effects of 2MBC. Notably, 2MBC can be generated in a gut-microbiota-dependent manner, whereas the accumulation of plasma 2MBC and its thrombosis-aggravating effect are largely ameliorated following antibiotic-induced microbial depletion. Our study implicates 2MBC as a metabolite that links gut microbiota dysbiosis to elevated thrombotic risk, providing mechanistic insight and a potential therapeutic strategy for thrombosis.
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