Major vault protein in cardiac and smooth muscle

N. Shults, Dividutta Das, Yuichiro J. Suzuki
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引用次数: 4

Abstract

Major vault protein (MVP) is the major component of the vault particle whose functions are not well understood. One proposed function of the vault is to serve as a mechanism of drug transport, which confers drug resistance in cancer cells. We show that MVP can be found in cardiac and smooth muscle. In human airway smooth muscle cells, knocking down MVP was found to cause cell death, suggesting that MVP serves as a cell survival factor. Further, our laboratory found that MVP is S-glutathionylated in response to ligand/receptor-mediated cell signaling. The S-glutathionylation of MVP appears to regulate protein-protein interactions between MVP and a protein called myosin heavy chain 9 (MYH9). Through MYH9 and Vsp34, MVP may form a complex with Beclin-1 that regulates autophagic cell death. In pulmonary vascular smooth muscle, proteasome inhibition promotes the ubiquitination of MVP, which may function as a mechanism of proteasome inhibition-mediated cell death. Investigating the functions and the regulatory mechanisms of MVP and vault particles is an exciting new area of research in cardiovascular/pulmonary pathophysiology.
心脏和平滑肌中的主要拱顶蛋白
主要拱顶蛋白(MVP)是拱顶颗粒的主要成分,其功能尚不清楚。一个被提出的拱顶的功能是作为药物运输的机制,这赋予癌细胞耐药性。我们发现MVP可以在心脏和平滑肌中发现。在人气道平滑肌细胞中,发现敲低MVP可导致细胞死亡,提示MVP是细胞存活因子。此外,我们的实验室发现MVP在响应配体/受体介导的细胞信号传导时被s -谷胱甘肽化。MVP的s -谷胱甘肽化似乎调节MVP和肌球蛋白重链9 (MYH9)之间的蛋白-蛋白相互作用。MVP可能通过MYH9和Vsp34与Beclin-1形成复合物,调控细胞自噬死亡。在肺血管平滑肌中,蛋白酶体抑制可促进MVP泛素化,这可能是蛋白酶体抑制介导细胞死亡的机制之一。研究MVP和拱顶颗粒的功能和调控机制是心血管/肺病理生理学研究的一个令人兴奋的新领域。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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