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热休克蛋白可增强细胞对凋亡的抗性。

Heat shock proteins increase resistance to apoptosis.

作者信息

Samali A, Cotter T G

机构信息

Department of Biochemistry, University College, Cork, Ireland.

出版信息

Exp Cell Res. 1996 Feb 25;223(1):163-70. doi: 10.1006/excr.1996.0070.

Abstract

Heat shock treatment of cells increases their survival and resistance to apoptosis. The kinetics of development of this resistance correlates with the kinetics of synthesis of heat shock proteins (hsps). U937 and Wehi-s cells were cultured for 1 h at 42 degrees C, conditions which induced the synthesis of heat shock proteins 27, 70, and 90. The cells were subsequently permitted to recover for a 2-h period, prior to exposure to the apoptosis inducing agents actinomycin-D (5 micrograms/ml), camptothecin (5 micrograms/ml), and etoposide (25 micrograms/ml). Apoptosis was determined by both DNA fragmentation and flow cytometric analysis. Heat-shocked cultures had a smaller number of apoptotic compared to control cultures when both were exposed to apoptosis inducing stimuli. Transfected Wehi-s cells constitutively overexpressing human hsp 70 or 27 were then examined for their resistance to apoptosis inducing by these drugs. Using the MTT assay, hsp 27 and 70 overexpressing cells exhibited an increased resistance to cell death when compared to the parental line. The parental line demonstrated features of apoptosis, that is, cell shrinkage and single- and double-strand DNA breaks. Taken together these results demonstrate that an increase in cellular levels of hsp 27 or 70, either by a mild heat shock treatment or by stable transfection, increases the resistance of U937 and Wehi-s cells to apoptotic cell death.

摘要

对细胞进行热休克处理可提高其存活率并增强抗凋亡能力。这种抗性的发展动力学与热休克蛋白(hsps)的合成动力学相关。将U937和Wehi-s细胞在42℃培养1小时,此条件可诱导热休克蛋白27、70和90的合成。随后让细胞恢复2小时,再暴露于凋亡诱导剂放线菌素-D(5微克/毫升)、喜树碱(5微克/毫升)和依托泊苷(25微克/毫升)。通过DNA片段化和流式细胞术分析来确定凋亡情况。当同时暴露于凋亡诱导刺激时,与对照培养物相比,热休克培养物中的凋亡细胞数量较少。然后检测持续过表达人hsp 70或27的转染Wehi-s细胞对这些药物诱导凋亡的抗性。使用MTT法,与亲代细胞系相比,过表达hsp 27和70的细胞对细胞死亡的抗性增加。亲代细胞系表现出凋亡特征,即细胞收缩以及单链和双链DNA断裂。综上所述,这些结果表明,通过温和的热休克处理或稳定转染使细胞内hsp 27或70水平升高,可增强U937和Wehi-s细胞对凋亡性细胞死亡的抗性。

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