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Subunit composition of mammalian transient receptor potential channels in living cells

机译:活细胞中哺乳动物瞬时受体电位通道的亚基组成

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摘要

Hormones, neurotransmitters, and growth factors give rise to calcium entry via receptor-activated cation channels that are activated downstream of phospholipase C activity. Members of the transient receptor potential channel (TRPC) family have been characterized as molecular substrates mediating receptor-activated cation influx. TRPC channels are assumed to be composed of multiple TRPC proteins. However, the cellular principles governing the assembly of TRPC proteins into homo- or heteromeric ion channels still remain elusive. By pursuing four independent experimental approaches—i.e., subcellular cotrafficking of TRPC subunits, differential functional suppression by dominant-negative subunits, fluorescence resonance energy transfer between labeled TRPC subunits, and coimmunoprecipitation—we investigate the combinatorial rules of TRPC assembly. Our data show that (i) TRPC2 does not interact with any known TRPC protein and (ii) TRPC1 has the ability to form channel complexes together with TRPC4 and TRPC5. (iii) All other TRPCs exclusively assemble into homo- or heterotetramers within the confines of TRPC subfamilies—e.g., TRPC4/5 or TRPC3/6/7. The principles of TRPC channel formation offer the conceptual framework to assess the physiological role of distinct TRPC proteins in living cells.
机译:激素,神经递质和生长因子通过受体激活的阳离子通道引起钙进入,该通道在磷脂酶C活性的下游被激活。瞬时受体电位通道(TRPC)家族的成员已被表征为介导受体激活的阳离子流入的分子底物。假定TRPC通道由多种TRPC蛋白组成。但是,控制TRPC蛋白组装成同型或异型离子通道的细胞原理仍然难以捉摸。通过采用四种独立的实验方法,即TRPC亚基的亚细胞共贩运,显性负亚基的功能差异抑制,标记的TRPC亚基之间的荧光共振能量转移以及共免疫沉淀,我们研究了TRPC组装的组合规则。我们的数据表明(i)TRPC2不与任何已知的TRPC蛋白相互作用,并且(ii)TRPC1具有与TRPC4和TRPC5一起形成通道复合物的能力。 (iii)所有其他TRPC仅在TRPC亚家族的范围内(例如TRPC4 / 5或TRPC3 / 6/7)组装成同型或异型四聚体。 TRPC通道形成的原理为评估活细胞中不同TRPC蛋白质的生理作用提供了概念框架。

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