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DEGRADATION OF SUBUNITS OF THE SEC61P COMPLEX, AN INTEGRAL COMPONENT OF THE ER MEMBRANE, BY THE UBIQUITIN-PROTEASOME PATHWAY

机译:SEC61P复杂的子单元退化ER膜的组成成分的UBIQUITIN-PROTEASOME通路

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摘要

We have investigated the degradation of subunits of the trimeric Sec61p complex, a key component of the protein translocation apparatus of the ER membrane, A mutant form of Sec61p and one of the two associated proteins (Sss1p) are selectively degraded, while the third constituent of the complex (Sbh1p) is stable, Our results demonstrate that the proteolysis of the multispanning membrane protein Sec61p is mediated by the ubiquitin-proteasome pathway, since it requires polyubiquitination, the presence of a membrane-bound (Ubc6) and a soluble (Ubc7) ubiquitin-conjugating enzyme and a functional proteasome. The process is proposed to be specific for unassembled Sec61p and Sss1p, Thus, our results suggest that one pathway of ER degradation of abnormal or unassembled membrane proteins is initiated at the cytoplasmic side of the ER.
机译:我们已经调查了子单元的退化的三聚物的Sec61p复杂,一个关键组件蛋白质的易位的装置膜的一种变异形式Sec61p之一两个相关的蛋白质(Sss1p)是选择性的退化,而第三个组成部分复杂的(Sbh1p)是稳定的,我们的结果证明的蛋白水解作用动静力膜蛋白Sec61p介导由ubiquitin-proteasome途径,因为它需要polyubiquitination,的存在膜结合(Ubc6)和可溶性(Ubc7)ubiquitin-conjugating酶和功能蛋白酶体。专门针对未装配的Sec61p Sss1p,因此,我们的研究结果表明,ER的途径之一退化的异常或未装配的膜蛋白质在细胞质端发起的有。

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