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热休克蛋白70B'的调控与功能。

Hsp70B' regulation and function.

作者信息

Noonan Emily J, Place Robert F, Giardina Charles, Hightower Lawrence E

机构信息

Department of Molecular and Cell Biology, University of Connecticut, Storrs, CT 06269-3125, USA.

出版信息

Cell Stress Chaperones. 2007 Winter;12(4):393-402. doi: 10.1379/csc-278e.1.

Abstract

Heat shock protein (Hsp) 70B' is a human Hsp70 chaperone that is strictly inducible, having little or no basal expression levels in most cells. Using siRNAs to knockdown Hsp70B' and Hsp72 in HT-29, SW-480, and CRL-1807 human colon cell lines, we have found that the two are regulated coordinately in response to stress. We also have found that proteasome inhibition is a potent activator of hsp70B'. Flow cytometry was used to assay hsp70B' promoter activity in HT-29eGFP cells in this study. Knockdown of both Hsp70B' and Hsp72 sensitized cells to heat stress and increasing concentrations of proteasome inhibitor. These data support the conclusion that Hsp72 is the primary Hsp70 family responder to increasing levels of proteotoxic stress, and Hsp70B' is a secondary responder. Interestingly ZnSO4 induces Hsp70B' and not Hsp72 in CRL-1807 cells, suggesting a stressor-specific primary role for Hsp70B'. Both Hsp70B' and Hsp72 are important for maintaining viability under conditions that increase the accumulation of damaged proteins in HT-29 cells. These findings are likely to be important in pathological conditions in which Hsp70B' contributes to cell survival.

摘要

热休克蛋白(Hsp)70B'是一种人类Hsp70伴侣蛋白,具有严格的诱导性,在大多数细胞中基础表达水平很低或几乎没有。通过使用小干扰RNA(siRNA)敲低HT - 29、SW - 480和CRL - 1807人结肠癌细胞系中的Hsp70B'和Hsp72,我们发现二者在应激反应中是协同调节的。我们还发现蛋白酶体抑制是hsp70B'的一种有效激活剂。在本研究中,使用流式细胞术检测HT - 29eGFP细胞中hsp70B'启动子活性。敲低Hsp70B'和Hsp72均使细胞对热应激和蛋白酶体抑制剂浓度增加敏感。这些数据支持以下结论:Hsp72是Hsp70家族对蛋白毒性应激水平升高的主要应答者,而Hsp70B'是次要应答者。有趣的是,硫酸锌在CRL - 1807细胞中诱导Hsp70B'而非Hsp72,表明Hsp70B'具有应激源特异性的主要作用。在增加HT - 29细胞中受损蛋白积累的条件下,Hsp70B'和Hsp72对维持细胞活力都很重要。这些发现可能在Hsp70B'有助于细胞存活的病理状况中具有重要意义。

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