Redondo Pedro C, Harper Alan G S, Salido Ginés M, Pariente Jose A, Sage Stewart O, Rosado Juan A
Department of Physiology, University of Extremadura, Cáceres, Spain.
J Physiol. 2004 Jul 1;558(Pt 1):99-109. doi: 10.1113/jphysiol.2004.064899. Epub 2004 Apr 30.
Store-mediated Ca2+ entry (SMCE) is a major mechanism for Ca2+ influx in non-excitable cells. Recently, a conformational coupling mechanism allowing coupling between transient receptor potential channels (TRPCs) and IP3 receptors has been proposed to activate SMCE. Here we have investigated the role of two soluble N-ethylmaleimide-sensitive-factor attachment protein receptors (SNAREs), which are involved in membrane trafficking and docking, in SMCE in human platelets. We found that the synaptosome-associated protein (SNAP-25) and the vesicle-associated membrane proteins (VAMP) coimmunoprecipitate with hTRPC1 in platelets. Treatment with botulinum toxin (BoNT) E or with tetanus toxin (TeTx), induced cleavage and inactivation of SNAP-25 and VAMPs, respectively. BoNTs significantly reduced thapsigargin- (TG) and agonist-evoked SMCE. Treatment with BoNTs once SMCE had been activated decreased Ca2+ entry, indicating that SNAP-25 is required for the activation and maintenance of SMCE. In contrast, treatment with TeTx had no effect on either the activation or the maintenance of SMCE in platelets. Finally, treatment with BoNT E impaired the coupling between naturally expressed hTRPC1 and IP3 receptor type II in platelets. From these findings we suggest SNAP-25 has a role in SMCE in human platelets.
储存介导的Ca2+内流(SMCE)是不可兴奋细胞中Ca2+流入的主要机制。最近,一种允许瞬时受体电位通道(TRPCs)与IP3受体偶联的构象偶联机制被提出用于激活SMCE。在此,我们研究了两种参与膜运输和对接的可溶性N-乙基马来酰亚胺敏感因子附着蛋白受体(SNAREs)在人血小板SMCE中的作用。我们发现,突触体相关蛋白(SNAP-25)和囊泡相关膜蛋白(VAMP)在血小板中与hTRPC1共同免疫沉淀。用肉毒杆菌毒素(BoNT)E或破伤风毒素(TeTx)处理分别诱导SNAP-25和VAMP的切割和失活。BoNTs显著降低了毒胡萝卜素(TG)和激动剂诱发的SMCE。在SMCE激活后用BoNTs处理会减少Ca2+内流,表明SNAP-25是SMCE激活和维持所必需的。相反,用TeTx处理对血小板中SMCE的激活或维持均无影响。最后,用BoNT E处理会损害血小板中天然表达的hTRPC1与II型IP3受体之间的偶联。从这些发现中我们认为SNAP-25在人血小板的SMCE中起作用。