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Structural order in Pannexin 1 cytoplasmic domains

机译:Pannexin 1细胞质结构域中的结构顺序

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Pannexin 1 forms ion and metabolite permeable hexameric channels with abundant expression in the central nervous system and elsewhere. Although pannexin 1 does not form intercellular channels, a common channel topology and oligomerization state, as well as involvement of the intracellular carboxyl terminal (CT) domain in channel gating, is shared with connexins. In this study, we characterized the secondary structure of the mouse pannexin 1 cytoplasmic domains to complement structural studies of the transmembrane segments and compare with similar domains from connexins. A combination of structural prediction tools and circular dichroism revealed that, unlike connexins (predominately intrinsically disordered), cytosolic regions of pannexin 1 contain approximately 50% secondary structure, a majority being α-helical. Moreover, prediction of transmembrane domains uncovered a potential membrane interacting region (I360-G370) located upstream of the caspase cleavage site (D375-D378) within the pannexin 1 CT domain. The α-helical content of a peptide containing these domains (G357-S384) increased in the presence of detergent micelles providing evidence of membrane association. We also purified a pannexin 1 CT construct containing the caspase cleavage site (M374-C426), assigned the resonances by NMR, and confirmed cleavage by Caspase-3 in vitro. On the basis of these structural studies of the cytoplasmic domains of pannexin 1, we propose a mechanism for the opening of pannexin 1 channels upon apoptosis, involving structural changes within the CT domain.
机译:Pannexin 1形成离子和代谢物可渗透的六聚体通道,在中枢神经系统和其他部位具有丰富的表达。尽管pannexin 1不形成细胞间通道,但连接蛋白具有共同的通道拓扑结构和低聚状态,以及细胞内羧基末端(CT)域参与通道门控。在这项研究中,我们表征了小鼠pannexin 1细胞质域的二级结构,以补充跨膜片段的结构研究,并与连接蛋白的相似域进行比较。结构预测工具和圆二色性的组合显示,与连接蛋白(主要是内在无序的)不同,pannexin 1的胞质区域包含约50%的二级结构,大部分为α螺旋。此外,对跨膜结构域的预测揭示了在泛新蛋白1 CT结构域内位于半胱天冬酶裂解位点(D375-D378)上游的潜在膜相互作用区域(I360-G370)。在存在洗涤剂胶束的情况下,包含这些结构域的肽(G357-S384)的α-螺旋含量增加,从而提供了膜缔合的证据。我们还纯化了含有caspase裂解位点(M374-C426)的pannexin 1 CT构建体,通过NMR分配了共振,并在体外证实了Caspase-3的裂解。在对pannexin 1胞质域的这些结构研究的基础上,我们提出了一种在凋亡时打开pannexin 1通道的机制,涉及CT域内的结构变化。

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