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铜(I)负载的 hCCS 结构域 1 的溶液结构解析 hSOD1 成熟的机制及无二硫键 hSOD1 突变体分析。

Mechanistic aspects of hSOD1 maturation from the solution structure of Cu(I) -loaded hCCS domain 1 and analysis of disulfide-free hSOD1 mutants.

机构信息

Magnetic Resonance Center (CERM), University of Florence, Via L. Sacconi 6, 50019 Sesto Fiorentino (Italy); Department of Chemistry, University of Florence, Via della Lastruccia 3, 50019 Sesto Fiorentino (Italy); Fondazione Farmacogenomica FiorGen onlus Via L. Sacconi 6, 50019, Sesto Fiorentino (Italy).

出版信息

Chembiochem. 2013 Sep 23;14(14):1839-44. doi: 10.1002/cbic.201300042. Epub 2013 Apr 26.

Abstract

Superoxide dismutase 1 (SOD1) maturation within the cell is mainly accomplished with the SOD1-specific chaperone, CCS, a dimeric protein with three distinct domains in each monomer. We recently showed that the first domain of human CCS (hCCSD1) is responsible for copper transfer to its protein partner, human SOD1 (hSOD1). The NMR solution structure of the copper(I)-loaded form of hCCSD1 reported here contributes further to characterization of the copper-transfer mechanism to hSOD1. NMR spectroscopy was also used to examine the hSOD1 mutants C57A, C146A, and C57A/C146A, which are unable to form the structurally conserved disulfide bond in SOD1, in order to investigate the role of these cysteines during hSOD1 copper acquisition. Together, the information on both hCCS and hSOD1, along with a sequence analysis of eukaryotic CCSD1, allows us to propose important mechanistic aspects regarding the copper-transfer process from hCCS to hSOD1.

摘要

细胞内超氧化物歧化酶 1(SOD1)的成熟主要通过 SOD1 特异性伴侣 CCS 完成,CCS 是一种具有三个独特结构域的二聚体蛋白。我们最近表明,人 CCS 的第一个结构域(hCCSD1)负责将铜转移到其蛋白伴侣人 SOD1(hSOD1)上。这里报道的铜(I)负载形式的 hCCSD1 的 NMR 溶液结构进一步有助于阐明向 hSOD1 转移铜的机制。NMR 光谱也用于研究无法形成 SOD1 中结构保守二硫键的 hSOD1 突变体 C57A、C146A 和 C57A/C146A,以研究这些半胱氨酸在 hSOD1 铜获取过程中的作用。综上所述,关于 hCCS 和 hSOD1 的信息,以及真核 CCSD1 的序列分析,使我们能够提出关于 hCCS 向 hSOD1 转移铜的重要机制方面。

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