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首页> 外文期刊>Frontiers in Molecular Biosciences >Structure of the Complete Dimeric Human GDAP1 Core Domain Provides Insights into Ligand Binding and Clustering of Disease Mutations
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Structure of the Complete Dimeric Human GDAP1 Core Domain Provides Insights into Ligand Binding and Clustering of Disease Mutations

机译:完整的二聚体人GDAP1核心结构域的结构提供了与疾病突变的配体结合和聚类的见解

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摘要

Charcot-Marie-Tooth disease (CMT) is one of the most common inherited neurological disorders. Despite the common involvement of ganglioside-induced differentiation-associated protein 1 (GDAP1) in CMT, the protein structure and function, as well as the pathogenic mechanisms, remain unclear. We determined the crystal structure of the complete human GDAP1 core domain, which shows a novel mode of dimerization within the glutathione S-transferase (GST) family. The long GDAP1-specific insertion forms an extended helix and a flexible loop. GDAP1 is catalytically inactive towards classical GST substrates. Through metabolite screening, we identified a ligand for GDAP1, the fatty acid hexadecanedioic acid, which is relevant for mitochondrial membrane permeability and Ca2 homeostasis. The fatty acid binds to a pocket next to a CMT-linked residue cluster, increases protein stability, and induces changes in protein conformation and oligomerization. The closest homologue of GDAP1, GDAP1L1, is monomeric in its full-length form. Our results highlight the uniqueness of GDAP1 within the GST family and point towards allosteric mechanisms in regulating GDAP1 oligomeric state and function.
机译:Charcot-Marie-Doother疾病(CMT)是最常见的遗传性神经系统疾病之一。尽管神经节苷脂诱导的分化相关蛋白1(GDAP1)在CMT中常见涉及CMT,蛋白质结构和功能以及致病机制仍然不清楚。我们确定了完整的人GDAP1核结构域的晶体结构,其显示了谷胱甘肽S-转移酶(GST)家族内的新型二聚化模式。长GDAP1特定插入形成延长的螺旋和柔性环。 GDAP1致常态GST基板催化不活性。通过代谢物筛选,我们鉴定了GDAP1的配体,脂肪酸十六烷基甲酸,其与线粒体膜渗透性和CA2稳态相关。脂肪酸与CMT连接的残余物簇旁边的口袋结合,增加蛋白质稳定性,并诱导蛋白质构象和寡聚化的变化。 GDAP1,GDAP1L1的最近同源物在其全长形式中是单体的。我们的结果突出了GDAP1在GST系列内的唯一性,并指向调节GDAP1低聚状态和功能的变构机制。

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