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ATP酶家族的一个新成员对于酿酒酵母中线粒体呼吸链和ATP合酶复合体的组装至关重要。

A new member of a family of ATPases is essential for assembly of mitochondrial respiratory chain and ATP synthetase complexes in Saccharomyces cerevisiae.

作者信息

Tzagoloff A, Yue J, Jang J, Paul M F

机构信息

Department of Biological Sciences, Columbia University, New York, New York 10027.

出版信息

J Biol Chem. 1994 Oct 21;269(42):26144-51.

PMID:7929327
Abstract

Respiration-defective pet mutants of Saccharomyces cerevisiae, assigned to complementation group G25, are grossly deficient in mitochondrial respiratory and ATPase complexes. This phenotype is usually found in strains impaired in mitochondrial protein synthesis. The G25 mutants, however, synthesize all of the proteins encoded by mitochondrial DNA. The mutants are also able to import and process cytoplasmically derived subunits of these enzymes. These results are most compatible with the idea that the gene defined by G25 mutants (RCA1) codes for a protein essential for the assembly of functional respiratory and ATPase complexes. The RCA1 gene has been cloned by complementation of an rca1 mutant with a yeast genomic library. The sequence of the encoded product shows Rca1 protein to be a new member of a recently described family of ATPases. The Rca1 protein is a mitochondrial membrane protein and is the third known member of this family implicated to function in the biogenesis of mitochondria. The primary structure of Rca1 protein indicates several distinct domains in addition to the common purine nucleotide binding region shared by all members of this protein family. One, located in the amino-terminal half, contains two hydrophobic stretches of sufficient length to span a membrane lipid bilayer.

摘要

酿酒酵母的呼吸缺陷型pet突变体被归为互补群G25,其线粒体呼吸和ATP酶复合体严重缺乏。这种表型通常出现在线粒体蛋白质合成受损的菌株中。然而,G25突变体能够合成线粒体DNA编码的所有蛋白质。这些突变体还能够导入并加工这些酶的细胞质衍生亚基。这些结果与以下观点最为相符,即由G25突变体定义的基因(RCA1)编码一种对功能性呼吸和ATP酶复合体组装至关重要的蛋白质。通过用酵母基因组文库互补rca1突变体,RCA1基因已被克隆。编码产物的序列显示Rca1蛋白是最近描述的ATP酶家族的一个新成员。Rca1蛋白是一种线粒体膜蛋白,是该家族中第三个被认为在线粒体生物发生中起作用的成员。Rca1蛋白的一级结构表明,除了该蛋白家族所有成员共有的常见嘌呤核苷酸结合区域外,还有几个不同的结构域。其中一个位于氨基末端的一半,包含两个足够长的疏水片段,足以跨越膜脂双层。

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