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首页> 外文期刊>The Biochemical Journal >Domain assembly of NAADP-gated two-pore channels.
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Domain assembly of NAADP-gated two-pore channels.

机译:NAADP门控两孔通道的结构域组装。

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摘要

TPCs (two-pore channels) have recently been identified as targets for the Ca2+-mobilizing messenger NAADP (nicotinic acid-adenine dinucleotide phosphate). TPCs have a unique structure consisting of cytosolic termini, two hydrophobic domains (I and II) each comprising six transmembrane regions and a pore, and a connecting cytosolic loop; however, little is known concerning how these channels are assembled. In the present paper, we report that both domain I and II of human TPCs are capable of independent insertion into membranes, whereas the loop linking the domains fails to insert. Pairs of transmembrane regions within domain I of TPC1 are also capable of insertion, consistent with sequential translational integration of hydrophobic regions. Insertion of the first two transmembrane regions, however, was inefficient, indicating possible interaction between transmembrane regions during translation. Both domains, and each pair of transmembrane regions within domain I, were capable of forming oligomers, highlighting marked redundancy in the molecular determinants driving oligomer formation. Each hydrophobic domain formed dimers upon cross-linking. The first four transmembrane regions of TPC1 also formed dimers, whereas transmembrane regions 5 and 6, encompassing the pore loop, formed both dimers and tetramers. TPCs thus probably assemble as dimers through differential interactions between transmembrane regions. The present study provides new molecular insight into the membrane insertion and oligomerization of TPCs.
机译:TPC(两孔通道)最近已被确定为可移动Ca2 +的信使NAADP(烟酸-腺嘌呤二核苷酸磷酸)的靶标。 TPC具有独特的结构,该结构由胞质末端,两个疏水域(I和II)组成,每个域包含六个跨膜区域和一个孔,以及一个连接的胞质环;然而,关于这些通道的组装方式知之甚少。在本文中,我们报道了人TPC的结构域I和II都能够独立插入膜中,而连接这些结构域的环却无法插入。 TPC1结构域I内的跨膜区对也能够插入,这与疏水区的顺序翻译整合一致。然而,前两个跨膜区的插入效率低下,表明翻译期间跨膜区之间可能存在相互作用。两个结构域以及结构域I内的每对跨膜区域均能够形成低聚物,从而突出显示了驱动低聚物形成的分子决定簇中的显着冗余。每个疏水域在交联时形成二聚体。 TPC1的前四个跨膜区域也形成二聚体,而包围孔环的跨膜区域5和6同时形成二聚体和四聚体。因此,TPC可能通过跨膜区域之间的不同相互作用组装成二聚体。本研究为TPC的膜插入和低聚提供了新的分子见解。

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