Structure-Function Comparisons of the Proapoptotic Protein Bax in Yeast and Mammalian Cells

生物 线粒体 Bcl-2相关X蛋白 细胞毒性T细胞 细胞生物学 酿酒酵母 酵母 细胞凋亡 突变体 分子生物学 程序性细胞死亡 生物化学 体外 基因 半胱氨酸蛋白酶3
作者
Hongbin Zha,Harold A. Fisk,Michael P. Yaffe,Nupam P. Mahajan,Brian Herman,John C. Reed
出处
期刊:Molecular and Cellular Biology [Taylor & Francis]
卷期号:16 (11): 6494-6508 被引量:283
标识
DOI:10.1128/mcb.16.11.6494
摘要

Expression of the proapoptotic protein Bax under the control of a GAL10 promoter in Saccharomyces cerevisiae resulted in galactose-inducible cell death. Immunofluorescence studies suggested that Bax is principally associated with mitochondria in yeast cells. Removal of the carboxyl-terminal transmembrane (TM) domain from Bax [creating Bax (deltaTM)] prevented targeting to mitochondrial and completely abolished cytotoxic function in yeast cells, suggesting that membrane targeting is crucial for Bax-mediated lethality. Fusing a TM domain from Mas70p, a yeast mitochondrial outer membrane protein, to Bax (deltaTM) restored targeting to mitochondria and cytotoxic function in yeast cells. Deletion of four well-conserved amino acids (IGDE) from the BH3 domain of Bax ablated its ability to homodimerize and completely abrogated lethality in yeast cells. In contrast, several Bax mutants which retained ability to homodimerize (deltaBH1, deltaBH2, and delta1-58) also retained at least partial lethal function in yeast cells. In coimmunoprecipitation experiments, expression of the wild-type Bax protein in Rat-1 fibroblasts and 293 epithelial cells induced apoptosis, whereas the Bax (deltaIGDE) mutant failed to induce apoptosis and did not associate with endogenous wild-type Bax protein. In contrast to yeast cells, Bax (deltaTM) protein retained cytotoxic function in Rat-1 and 293 cells, was targeted largely to mitochondria, and dimerized with endogenous Bax in mammalian cells. Thus, the dimerization-mediating BH3 domain and targeting to mitochondrial membranes appear to be essential for the cytotoxic function of Bax in both yeast and mammalian cells.

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