两种主要的泛素受体在蛋白酶体中的功能差异；S5a 和 hRpn13。

Functional differences between two major ubiquitin receptors in the proteasome; S5a and hRpn13.

机构信息

School of Life Sciences, Gwangju Institute of Science & Technology, 1 Oryong-dong Buk-ku, Gwangju 500-712, Republic of Korea.

出版信息

Biochem Biophys Res Commun. 2010 May 28;396(2):425-8. doi: 10.1016/j.bbrc.2010.04.108. Epub 2010 Apr 22.

DOI:10.1016/j.bbrc.2010.04.108

PMID:20417181

Abstract

It is well known that S5a and hRpn13 are two major ubiquitin (Ub) receptors in the proteasome but little is known about their functional difference in recruiting ubiquitinated substrates. In this study using siRNA-mediated knockdown of S5a or hRpn13, we found that two Ub receptors had different substrate specificity although similar level of accumulation of high molecular weight Ub-conjugates was observed. Interesting enough, depletion of S5a, but not hRpn13, resulted in the Ub-containing aggregates and induced ER chaperones such as Grp78 and Grp94. ERAD substrates such as alpha-TCR and alpha1-antitrypsin were also stabilized by the depletion of S5a but not hRpn13. Our results suggest that there is different substrate specificity between S5a and hRpn13 at the level of delivery and S5a may be the major docking site for ERAD substrates.

摘要

众所周知，S5a 和 hRpn13 是蛋白酶体中的两个主要泛素（Ub）受体，但关于它们在募集泛素化底物方面的功能差异知之甚少。在本研究中，我们使用 siRNA 介导的 S5a 或 hRpn13 敲低，发现虽然观察到高分子量 Ub 缀合物的积累水平相似，但两种 Ub 受体具有不同的底物特异性。有趣的是，S5a 的耗竭而不是 hRpn13 的耗竭导致含有 Ub 的聚集体的形成，并诱导 ER 伴侣蛋白，如 Grp78 和 Grp94。S5a 的耗竭而非 hRpn13 的耗竭也稳定了 ERAD 底物，如 alpha-TCR 和 alpha1-抗胰蛋白酶。我们的结果表明，在递呈水平上 S5a 和 hRpn13 之间存在不同的底物特异性，S5a 可能是 ERAD 底物的主要对接位点。

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两种主要的泛素受体在蛋白酶体中的功能差异；S5a 和 hRpn13。

Functional differences between two major ubiquitin receptors in the proteasome; S5a and hRpn13.

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