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酿酒酵母中铜输出在分泌途径中被限制于晚期高尔基体或高尔基体后区室。

Restriction of copper export in Saccharomyces cerevisiae to a late Golgi or post-Golgi compartment in the secretory pathway.

作者信息

Yuan D S, Dancis A, Klausner R D

机构信息

Cell Biology and Metabolism Branch, NICHD, National Institutes of Health, Bethesda, Maryland 20892, USA.

出版信息

J Biol Chem. 1997 Oct 10;272(41):25787-93. doi: 10.1074/jbc.272.41.25787.

Abstract

The CCC2 gene in the yeast Saccharomyces cerevisiae encodes a P-type ATPase (Ccc2p) required for the export of cytosolic copper to the extracytosolic domain of a copper-dependent oxidase, Fet3p. Ccc2p appears to be both a structural and functional homolog of ATPases impaired in two human disorders of intracellular copper transport, Menkes disease and Wilson disease. In the present work, three approaches were used to determine the locus of Ccc2p-dependent copper export within the secretory pathway. First, like ccc2 mutants, sec mutants blocked in the secretory pathway at steps prior to and including the Golgi complex failed to deliver radioactive copper to Fet3p. Second, also like ccc2 mutants, vps33 and certain other mutants with defects in post-Golgi sorting exhibited phenotypes traceable to deficient copper delivery to Fet3p. These findings were sufficient to explain the respiratory deficiency of these mutants. Third, immunofluorescence microscopy revealed that Ccc2p was distributed among several punctate foci within wild-type cells, consistent with late Golgi or post-Golgi localization. Thus, copper export by Ccc2p appears to be restricted to a late or post-Golgi compartment in the secretory pathway.

摘要

酿酒酵母中的CCC2基因编码一种P型ATP酶(Ccc2p),该酶是将胞质铜输出到铜依赖性氧化酶Fet3p的胞外区域所必需的。Ccc2p似乎是两种人类细胞内铜转运疾病(门克斯病和威尔逊病)中功能受损的ATP酶的结构和功能同源物。在本研究中,采用了三种方法来确定分泌途径中Ccc2p依赖性铜输出的位点。首先,与ccc2突变体一样,在分泌途径中高尔基体复合体之前及包括高尔基体复合体在内的步骤被阻断的sec突变体无法将放射性铜传递给Fet3p。其次,同样与ccc2突变体一样,vps33和其他一些在高尔基体后分选存在缺陷的突变体表现出可追溯到铜传递给Fet3p不足的表型。这些发现足以解释这些突变体的呼吸缺陷。第三,免疫荧光显微镜显示,Ccc2p分布在野生型细胞内的几个点状病灶中,这与高尔基体晚期或高尔基体后定位一致。因此,Ccc2p介导的铜输出似乎局限于分泌途径中的高尔基体晚期或高尔基体后区室。

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