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血影蛋白的泛素化调节红细胞血影蛋白-蛋白4.1-肌动蛋白三元复合物的解离:对镰状细胞膜骨架的影响。

Ubiquitination of spectrin regulates the erythrocyte spectrin-protein-4.1-actin ternary complex dissociation: implications for the sickle cell membrane skeleton.

作者信息

Ghatpande S S, Goodman S R

机构信息

Department of Molecular and Cell Biology, University of Texas at Dallas, Richardson, TX, USA.

出版信息

Cell Mol Biol (Noisy-le-grand). 2004 Feb;50(1):67-74.

Abstract

It has been demonstrated by our laboratory that the irreversibly sickled cell (ISC) spectrin-4.1-actin complex dissociates slowly as compared to ternary complexes formed out of control (AA) and reversibly sickle cell (RSCs) core skeletons. These studies indicated that the molecular basis for the inability of irreversibly sickled cells (ISCs) to change shape is a skeleton that disassembles, and therefore reassembles, very slowly. The present study is based on the following observations: a) alpha-spectrin repeats 20 and 21 contain ubiquitination sites, and b) The spectrin repeats beta-1 and beta-2 are in direct contact with spectrin repeats alpha-20 and alpha-21 during spectrin heterodimer formation, and contain the protein 4.1 binding domain. We demonstrate here that alpha-spectrin ubiquitination at repeats 20 and 21 increases the dissociation of the spectrin-protein-4.1-actin ternary complex thereby regulating protein 4.1's ability to stimulate the spectrin-actin interaction. Performing in vitro ternary complex dissociation assays with AA control and sickle cell SS spectrin (isolated from high-density sickle cells), we further demonstrate that reduced ubiquitination of alpha-spectrin is, in part, responsible for the locked membrane skeleton in sickle cell disease.

摘要

我们实验室已证明,与由对照(AA)和可逆性镰状细胞(RSC)核心骨架形成的三元复合物相比,不可逆性镰状细胞(ISC)的血影蛋白-4.1-肌动蛋白复合物解离缓慢。这些研究表明,不可逆性镰状细胞(ISC)无法改变形状的分子基础是一种拆卸和重新组装都非常缓慢的骨架。本研究基于以下观察结果:a)α-血影蛋白的第20和21个重复序列包含泛素化位点,b)在血影蛋白异二聚体形成过程中,血影蛋白β-1和β-2重复序列与血影蛋白α-20和α-21重复序列直接接触,并包含蛋白4.1结合结构域。我们在此证明,α-血影蛋白第20和21个重复序列的泛素化增加了血影蛋白-蛋白4.1-肌动蛋白三元复合物的解离,从而调节蛋白4.1刺激血影蛋白-肌动蛋白相互作用的能力。通过对AA对照和镰状细胞SS血影蛋白(从高密度镰状细胞中分离)进行体外三元复合物解离试验,我们进一步证明,α-血影蛋白泛素化减少在一定程度上导致了镰状细胞病中膜骨架的锁定。

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