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单体 CCTδ 与 p150 之间的相互作用:CCTδ 在细胞外周的一种新功能,与分子伴侣 CCT 的蛋白质折叠活性不同。

Interactions between monomeric CCTδ and p150: A novel function for CCTδ at the cell periphery distinct from the protein folding activity of the molecular chaperone CCT.

机构信息

Department of Chemistry and Molecular Biology, University of Gothenburg, 40530, Sweden.

Department of Chemistry and Molecular Biology, University of Gothenburg, 40530, Sweden.

出版信息

Exp Cell Res. 2018 Sep 1;370(1):137-149. doi: 10.1016/j.yexcr.2018.06.018. Epub 2018 Jun 18.

DOI:10.1016/j.yexcr.2018.06.018
PMID:29913154
Abstract

Chaperonin containing tailless complex polypeptide 1 (CCT) is a molecular chaperone consisting of eight distinct protein subunits, that when oligomeric is essential for the folding of newly synthesized tubulin and actin. In addition to folding, CCT activity includes functions of individual subunits in their monomeric form. For example, when CCTδ monomer levels are increased in cultured mammalian cells, numerous cell surface protrusions are formed from retraction fibres, indicating that an underlying function for the CCTδ monomer exists. Here, using a yeast two-hybrid screen we identify the dynactin complex component p150 as a binding partner for CCTδ and show by siRNA depletion that this interaction is required for the formation of CCTδ-induced cell surface protrusions. Intact microtubules are necessary for the formation of the protrusions, consistent with microtubule minus end transport driving the retraction fibre formation and depletion of either p150 or the dynactin complex-associated transmembrane protein dynAP prevents the previously observed localization of GFP-CCTδ to the plasma membrane. Wound healing assays reveal that CCTδ monomer levels influence directional cell migration and together our observations demonstrate that in addition to the folding activity of CCT in its oligomer form, a monomeric subunit is associated with events that involve the assembled cytoskeleton.

摘要

无尾复合物多肽 1(CCT)包含一个分子伴侣,由八个不同的蛋白质亚基组成,当形成寡聚体时,对于新合成的微管蛋白和肌动蛋白的折叠是必不可少的。除了折叠之外,CCT 的活性还包括其单体形式的各个亚基的功能。例如,当培养的哺乳动物细胞中 CCTδ 单体水平增加时,从回缩纤维形成许多细胞表面突起,表明 CCTδ 单体存在潜在的功能。在这里,我们使用酵母双杂交筛选鉴定出动力蛋白复合物成分 p150 是 CCTδ 的结合伴侣,并通过 siRNA 耗竭表明这种相互作用对于 CCTδ 诱导的细胞表面突起的形成是必需的。完整的微管对于突起的形成是必要的,这与微管负端运输驱动回缩纤维的形成一致,并且耗竭 p150 或动力蛋白复合物相关的跨膜蛋白 dynAP 可防止先前观察到的 GFP-CCTδ 到质膜的定位。划痕愈合实验表明 CCTδ 单体水平影响细胞的定向迁移,我们的观察结果共同表明,除了其寡聚体形式的折叠活性外,一个单体亚基与涉及组装细胞骨架的事件相关。

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