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质子离子载体可阻止过氧化物酶体蛋白的组装。

Proton ionophores prevent assembly of a peroxisomal protein.

作者信息

Bellion E, Goodman J M

出版信息

Cell. 1987 Jan 16;48(1):165-73. doi: 10.1016/0092-8674(87)90367-9.

Abstract

Peroxisomal matrix proteins are imported into the organelle posttranslationally. Here we report that proton ionophores disrupt the import and assembly of alcohol oxidase, a homo-octameric flavoprotein of the induced peroxisome from the methylotrophic yeast Candida boidinii. When drug is added to cells containing newly synthesized monomeric alcohol oxidase, octamerization fails to occur and a membrane-associated complex is formed instead. The formation of the complex, which appears to face the cytoplasmic side of the membrane, is reversed when drug is removed, leading to the generation of octamer. Surprisingly, when drug is added to cells containing newly assembled octamers, they dissociate into monomers. We suggest that both the complex and the labile octamer are intermediates in the normal assembly pathway of alcohol oxidase and that energy is required for import and maturation of this peroxisomal protein.

摘要

过氧化物酶体基质蛋白在翻译后被导入该细胞器。在此我们报告,质子离子载体破坏了醇氧化酶的导入和组装,醇氧化酶是来自甲基营养型酵母博伊丁假丝酵母的诱导过氧化物酶体中的一种同源八聚体黄素蛋白。当将药物添加到含有新合成的单体醇氧化酶的细胞中时,八聚化无法发生,而是形成了一种与膜相关的复合物。该复合物似乎面向膜的细胞质侧,当去除药物时其形成会逆转,从而导致八聚体的产生。令人惊讶的是,当将药物添加到含有新组装的八聚体的细胞中时,它们会解离成单体。我们认为复合物和不稳定的八聚体都是醇氧化酶正常组装途径中的中间体,并且这种过氧化物酶体蛋白的导入和成熟需要能量。

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