Tranter John D, Mikami Ryan T, Kumar Ashutosh, Brown Gavriel, Abd El-Aziz Tarek M, Zhao Yonghui, Abraham Nihil, Meyer Chloe, Ajanel Abigail, Xie Litao, Ashworth Katrina, Hong Juan, Zhang Haixia, Kumari Tripti, Balutowski Adam, Liu Alice, Bark David, Nair Vinayak K, Lasky Nina M, Feng Yongmei, Stitziel Nathan O, Lerner Daniel J, Campbell Robert A, Paola Jorge Di, Cho Jaehyung, Sah Rajan
bioRxiv. 2024 Sep 26:2024.09.26.615233. doi: 10.1101/2024.09.26.615233.
Platelet shape and volume changes are early mechanical events contributing to platelet activation and thrombosis. Here, we identify single-nucleotide polymorphisms in Leucine-Rich Repeat Containing 8 (LRRC8) protein subunits that form the Volume-Regulated Anion Channel (VRAC) which are independently associated with altered mean platelet volume. LRRC8A is required for functional VRAC in megakaryocytes (MKs) and regulates platelet volume, adhesion, and agonist-stimulated activation, aggregation, ATP secretion and calcium mobilization. MK-specific LRRC8A cKO mice have reduced arteriolar thrombus formation and prolonged arterial thrombosis without affecting bleeding times. Mechanistically, platelet LRRC8A mediates swell-induced ATP/ADP release to amplify agonist-stimulated calcium and PI3K-AKT signaling via P2X1, P2Y and P2Y receptors. Small-molecule LRRC8 channel inhibitors recapitulate defects observed in LRRC8A-null platelets and . These studies identify the mechanoresponsive LRRC8 channel complex as an ATP/ADP release channel in platelets which regulates platelet function and thrombosis, providing a proof-of-concept for a novel anti-thrombotic drug target.
血小板形状和体积变化是促成血小板活化和血栓形成的早期机械事件。在此,我们鉴定出富含亮氨酸重复序列8(LRRC8)蛋白亚基中的单核苷酸多态性,这些亚基形成容积调节性阴离子通道(VRAC),它们独立地与平均血小板体积改变相关。LRRC8A是巨核细胞(MKs)中功能性VRAC所必需的,并调节血小板体积、黏附以及激动剂刺激的活化、聚集、ATP分泌和钙动员。MK特异性LRRC8A基因敲除小鼠的小动脉血栓形成减少,动脉血栓形成时间延长,而不影响出血时间。从机制上讲,血小板LRRC8A介导肿胀诱导的ATP/ADP释放,以通过P2X1、P2Y和P2Y受体放大激动剂刺激的钙和PI3K-AKT信号传导。小分子LRRC8通道抑制剂重现了在LRRC8A缺失血小板中观察到的缺陷。这些研究确定了机械反应性LRRC8通道复合物作为血小板中的ATP/ADP释放通道,其调节血小板功能和血栓形成,为新型抗血栓药物靶点提供了概念验证。
