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在铜转运蛋白中发现的一种Mets基序肽仅通过甲硫氨酸配位选择性结合Cu(I)。

A Mets motif peptide found in copper transport proteins selectively binds Cu(I) with methionine-only coordination.

作者信息

Jiang Jianfeng, Nadas Istvan A, Kim M Alison, Franz Katherine J

机构信息

Department of Chemistry, Duke University, P.O. Box 90346, Durham, North Carolina 27708, USA.

出版信息

Inorg Chem. 2005 Dec 26;44(26):9787-94. doi: 10.1021/ic051180m.

Abstract

Mets motifs, which refer to methionine-rich sequences found in the high-affinity copper transporter Ctr1, also appear in other proteins involved in copper trafficking and homeostasis, including other Ctrs as well as Pco and Cop proteins isolated from copper-resistant bacteria. To understand the coordination chemistry utilized by these proteins, we studied the copper binding properties of a peptide labeled Mets7-PcoC with the sequence Met-Thr-Gly-Met-Lys-Gly-Met-Ser. By comparing this sequence to a series of mutants containing noncoordinating norleucine in place of methionine, we confirm that all three methionine residues are involved in a thioether-only binding site that is selective for Cu(I). Two independent methods, one based on mass spectrometry and one based on rate differences for the copper-catalyzed oxidation of ascorbic acid, provide an effective K(D) of approximately 2.5 microM at pH 4.5 for the 1:1 complex of Mets7-PcoC with Cu(I). These results establish that a relatively simple peptide containing an MX(2)MX(2)M motif is sufficient to bind Cu(I) with an affinity that corresponds well with its proposed biological function of extracellular copper acquisition.

摘要

Mets基序是指在高亲和力铜转运蛋白Ctr1中发现的富含甲硫氨酸的序列,它也出现在其他参与铜转运和稳态的蛋白质中,包括其他Ctr蛋白以及从耐铜细菌中分离出的Pco和Cop蛋白。为了了解这些蛋白质所利用的配位化学,我们研究了一种标记为Mets7-PcoC的肽的铜结合特性,其序列为Met-Thr-Gly-Met-Lys-Gly-Met-Ser。通过将该序列与一系列用非配位正亮氨酸取代甲硫氨酸的突变体进行比较,我们证实所有三个甲硫氨酸残基都参与了一个仅含硫醚的结合位点,该位点对Cu(I)具有选择性。两种独立的方法,一种基于质谱,另一种基于铜催化的抗坏血酸氧化的速率差异,在pH 4.5时,Mets7-PcoC与Cu(I)的1:1复合物的有效解离常数(K(D))约为2.5 microM。这些结果表明,一个含有MX(2)MX(2)M基序的相对简单的肽足以以与其提出的细胞外铜摄取生物学功能相匹配的亲和力结合Cu(I)。

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