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首页> 外文期刊>Structure >Crystal Structures of the N-Terminal Domains of Cardiac and Skeletal Muscle Ryanodine Receptors: Insights into Disease Mutations
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Crystal Structures of the N-Terminal Domains of Cardiac and Skeletal Muscle Ryanodine Receptors: Insights into Disease Mutations

机译:心脏和骨骼肌Ryanodine受体的N末端域的晶体结构:疾病突变的见解。

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摘要

Ryanodine receptors (RyRs) are channels governing the release of Ca2+ from the sarcoplasmic or endoplasmic reticulum. They are required for the contraction of both skeletal (RyR1) and cardiac (RyR2) muscles. Mutations in both RyR1 and RyR2 have been associated with severe genetic disorders, but high-resolution data describing the disease variants in detail have been lacking. Here we present the crystal structures of the N-terminal domains of both RyR2 (1-217) and RyR1 (9-205) at 2.55 angstrom and 2.9 angstrom, respectively. The domains map in a hot spot region for disease mutations. Both structures consist of a core beta trefoil domain flanked by an alpha helix. Crystal structures of two RYR2 disease mutants, A77V (2.2 angstrom) and V186M (1.7 angstrom), show that the mutations cause distinct local changes in the surface of the protein. A RyR2 deletion mutant causes significant changes in the thermal stability. The disease positions highlight two putative binding interfaces required for normal RyR function.
机译:Ryanodine受体(RyRs)是支配从肌浆网或内质网释放Ca2 +的通道。它们是骨骼肌(RyR1)和心肌(RyR2)收缩所必需的。 RyR1和RyR2的突变均与严重的遗传疾病有关,但缺乏详细描述疾病变异的高分辨率数据。在这里,我们介绍RyR2(1-217)和RyR1(9-205)N端域的晶体结构分别在2.55埃和2.9埃。这些域在热点区域中映射疾病突变。两种结构均由一个侧翼为α螺旋的核心β三叶结构域组成。两个RYR2疾病突变体A77V(2.2埃)和V186M(1.7埃)的晶体结构表明,这些突变引起蛋白质表面的明显局部变化。 RyR2缺失突变体引起热稳定性的显着变化。疾病位置突出了正常RyR功能所需的两个假定的结合界面。

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