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酵母细胞色素c氧化酶17的溶液结构及铜(I)结合

Yeast cox17 solution structure and Copper(I) binding.

作者信息

Abajian Carnie, Yatsunyk Liliya A, Ramirez Benjamin E, Rosenzweig Amy C

机构信息

Department of Biochemistry, Northwestern University, Evanston, IL 60208, USA.

出版信息

J Biol Chem. 2004 Dec 17;279(51):53584-92. doi: 10.1074/jbc.M408099200. Epub 2004 Oct 1.

DOI:10.1074/jbc.M408099200
PMID:15465825
Abstract

Cox17 is a 69-residue cysteine-rich, copper-binding protein that has been implicated in the delivery of copper to the Cu(A) and Cu(B) centers of cytochrome c oxidase via the copper-binding proteins Sco1 and Cox11, respectively. According to isothermal titration calorimetry experiments, fully reduced Cox17 binds one Cu(I) ion with a K(a) of (6.15 +/- 5.83) x 10(6) M(-1). The solution structures of both apo and Cu(I)-loaded Cox17 reveal two alpha helices preceded by an extensive, unstructured N-terminal region. This region is reminiscent of intrinsically unfolded proteins. The two structures are very similar overall with residues in the copper-binding region becoming more ordered in Cu(I)-loaded Cox17. Based on the NMR data, the Cu(I) ion has been modeled as two-coordinate with ligation by conserved residues Cys(23) and Cys(26). This site is similar to those observed for the Atx1 family of copper chaperones and is consistent with reported mutagenesis studies. A number of conserved, positively charged residues may interact with complementary surfaces on Sco1 and Cox11, facilitating docking and copper transfer. Taken together, these data suggest that Cox17 is not only well suited to a copper chaperone function but is specifically designed to interact with two different target proteins.

摘要

Cox17是一种含有69个氨基酸残基、富含半胱氨酸的铜结合蛋白,分别通过铜结合蛋白Sco1和Cox11将铜传递至细胞色素c氧化酶的Cu(A)和Cu(B)中心。根据等温滴定量热法实验,完全还原的Cox17以(6.15±5.83)×10⁶ M⁻¹的解离常数(K(a))结合一个Cu(I)离子。脱辅基和负载Cu(I)的Cox17的溶液结构均显示,在一个广泛的无结构N端区域之前有两个α螺旋。该区域让人联想到内在无序蛋白。两种结构总体上非常相似,在负载Cu(I)的Cox17中,铜结合区域的残基变得更加有序。基于核磁共振数据,Cu(I)离子已被模拟为与保守残基Cys(23)和Cys(26)形成双配位。该位点与铜伴侣蛋白Atx1家族中观察到的位点相似,并且与已报道的诱变研究结果一致。许多保守的带正电荷残基可能与Sco1和Cox11上的互补表面相互作用,促进对接和铜转移。综上所述,这些数据表明Cox17不仅非常适合发挥铜伴侣蛋白的功能,而且经过专门设计以与两种不同的靶蛋白相互作用。

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