BH3配体调节MCL-1与E3连接酶的结合。

BH3-ligand regulates access of MCL-1 to its E3 ligase.

作者信息

Warr Matthew R, Acoca Stephane, Liu Zhiqian, Germain Marc, Watson Mark, Blanchette Mathieu, Wing Simon S, Shore Gordon C

机构信息

Department of Biochemistry, McIntyre Medical Sciences Building, McGill University, Montréal, Que., Canada.

出版信息

FEBS Lett. 2005 Oct 24;579(25):5603-8. doi: 10.1016/j.febslet.2005.09.028. Epub 2005 Sep 28.

DOI:10.1016/j.febslet.2005.09.028

PMID:16213503

Abstract

A genome wide search for new BH3-containing Bcl-2 family members was conducted using position weight matrices (PWM) and identified a large (480kDa), novel BH3-only protein, originally called LASU1 (now also known as Ureb-1, E3(histone), ARF-BP1, and Mule). We demonstrated that LASU1 is an E3 ligase that ubiquitinated Mcl-1 in vitro and was required for its proteasome-dependent degradation in HeLa cells. Of note, the BH3 domain of LASU1 interacted with Mcl-1 but not with Bcl-2 or Bcl-Xl. A competing BH3-ligand derived from Bim interacted with Mcl-1 and prevented its interaction with LASU1 in HeLa cells, causing elevation of the steady-state levels of Mcl-1. This suggests that the unliganded form of Mcl-1 is sensitive to LASU1-mediated degradation of Mcl-1.

摘要

利用位置权重矩阵（PWM）进行全基因组搜索，以寻找新的含BH3结构域的Bcl-2家族成员，并鉴定出一种大型（480kDa）的新型仅含BH3结构域的蛋白质，最初称为LASU1（现也称为Ureb-1、E3（组蛋白）、ARF-BP1和Mule）。我们证明LASU1是一种E3连接酶，在体外可使Mcl-1泛素化，并且是HeLa细胞中其蛋白酶体依赖性降解所必需的。值得注意的是，LASU1的BH3结构域与Mcl-1相互作用，但不与Bcl-2或Bcl-Xl相互作用。源自Bim的竞争性BH3配体与Mcl-1相互作用，并阻止其在HeLa细胞中与LASU1相互作用，导致Mcl-1稳态水平升高。这表明未结合配体形式的Mcl-1对LASU1介导的Mcl-1降解敏感。

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BH3配体调节MCL-1与E3连接酶的结合。

BH3-ligand regulates access of MCL-1 to its E3 ligase.

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