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Two-pore channels at the intersection of endolysosomal membrane traffic

机译:溶酶体膜运输相交处的两孔通道

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摘要

Two-pore channels (TPCs) are ancient members of the voltage-gated ion channel superfamily that localize to acidic organelles such as lysosomes. The TPC complex is the proposed target of the Ca2 +-mobilizing messenger NAADP, which releases Ca2 + from these acidic Ca2 + stores. Whereas details of TPC activation and native ion permeation remain unclear, a consensus has emerged around their function in regulating endolysosomal trafficking. This role is supported by recent proteomic data showing that TPCs interact with proteins controlling membrane organization and dynamics, including Rab GTPases and components of the fusion apparatus. Regulation of TPCs by PtdIns(3,5)P2 and/or NAADP (nicotinic acid adenine dinucleotide phosphate) together with their functional and physical association with Rab proteins provides a mechanism for coupling phosphoinositide and trafficking protein cues to local ion fluxes. Therefore, TPCs work at the regulatory cross-roads of (patho)physiological cues to co-ordinate and potentially deregulate traffic flow through the endolysosomal network. This review focuses on the native role of TPCs in trafficking and their emerging contributions to endolysosomal trafficking dysfunction.
机译:两孔通道(TPC)是电压门控离子通道超家族的古老成员,其位于酸性细胞器(如溶酶体)中。 TPC复合物是Ca 2 + 动员信使NAADP的拟议目标,该信使NAADP从这些酸性Ca 2 + 存储中释放Ca 2 + 。 。虽然尚不清楚TPC活化和天然离子渗透的细节,但围绕它们在调节溶酶体运输中的功能已达成共识。最近的蛋白质组学数据表明TPC与控制膜组织和动力学的蛋白质相互作用,包括Rab GTPases和融合装置的组件,从而证明了这一作用。通过PtdIns(3,5)P2和/或NAADP(烟酸腺嘌呤二核苷酸磷酸)对TPC的调节,以及它们与Rab蛋白的功能和物理缔合,提供了一种将磷酸肌醇和蛋白提示运至局部离子通量的机制。因此,TPC在(病理)生理线索的调节十字路口工作,以协调和潜在地放松通过溶酶体网络的交通流量。这篇综述着重于TPC在贩运中的固有作用及其对溶酶体贩运功能障碍的新贡献。

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