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门克斯病/威尔逊病蛋白金属伴侣介导铜转运的结构基础。

Structural basis for copper transfer by the metallochaperone for the Menkes/Wilson disease proteins.

作者信息

Wernimont A K, Huffman D L, Lamb A L, O'Halloran T V, Rosenzweig A C

机构信息

Department of Biochemistry, Molecular Biology, and Cell Biology, Northwestern University, Evanston, Illinois 60208, USA.

出版信息

Nat Struct Biol. 2000 Sep;7(9):766-71. doi: 10.1038/78999.

Abstract

The Hah1 metallochaperone protein is implicated in copper delivery to the Menkes and Wilson disease proteins. Hah1 and the N-termini of its target proteins belong to a family of metal binding domains characterized by a conserved MT/HCXXC sequence motif. The crystal structure of Hah1 has been determined in the presence of Cu(I), Hg(II), and Cd(II). The 1.8 A resolution structure of CuHah1 reveals a copper ion coordinated by Cys residues from two adjacent Hah1 molecules. The CuHah1 crystal structure is the first of a copper chaperone bound to copper and provides structural support for direct metal ion exchange between conserved MT/HCXXC motifs in two domains. The structures of HgHah1 and CdHah1, determined to 1.75 A resolution, also reveal metal ion coordination by two MT/HCXXC motifs. An extended hydrogen bonding network, unique to the complex of two Hah1 molecules, stabilizes the metal binding sites and suggests specific roles for several conserved residues. Taken together, the structures provide models for intermediates in metal ion transfer and suggest a detailed molecular mechanism for protein recognition and metal ion exchange between MT/HCXXC containing domains.

摘要

Hah1金属伴侣蛋白参与向门克斯病和威尔逊病蛋白输送铜。Hah1及其靶蛋白的N端属于一个金属结合结构域家族,其特征是具有保守的MT/HCXXC序列基序。已在存在Cu(I)、Hg(II)和Cd(II)的情况下确定了Hah1的晶体结构。CuHah1的1.8埃分辨率结构显示一个铜离子由来自两个相邻Hah1分子的半胱氨酸残基配位。CuHah1晶体结构是与铜结合的铜伴侣蛋白的首个结构,为两个结构域中保守的MT/HCXXC基序之间的直接金属离子交换提供了结构支持。分辨率为1.75埃的HgHah1和CdHah1结构也显示了两个MT/HCXXC基序对金属离子的配位作用。两个Hah1分子复合物特有的一个延伸氢键网络稳定了金属结合位点,并表明了几个保守残基的特定作用。总之,这些结构为金属离子转移中间体提供了模型,并提出了含MT/HCXXC结构域之间蛋白质识别和金属离子交换的详细分子机制。

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