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首页> 外文期刊>American Journal of Physiology >Identification of the functional domain of p21(WAF1/CIP1) that protects cells from cisplatin cytotoxicity.
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Identification of the functional domain of p21(WAF1/CIP1) that protects cells from cisplatin cytotoxicity.

机译:鉴定保护细胞免受顺铂细胞毒性的p21(WAF1 / CIP1)功能域。

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摘要

The p21 cyclin-dependent kinase (cdk) inhibitor protects cells from cisplatin cytotoxicity in vivo and in vitro. However, the mechanism of protection is not known. Separate p21 domains are known to interact with several different proteins having proapoptotic functions. To investigate the mechanism of protection by p21, we have constructed adenoviruses encoding the different domains of p21. We were able to localize the protective activity to a region of 54 amino acids containing the cyclin-cdk interacting moiety. Other protein binding domains of p21, including the NH2-terminal procaspase-3 interactive region and the COOH-terminal region containing the proliferating cell nuclear antigen binding domain and the nuclear localization signal, had little protective effect on cisplatin cytotoxicity. The dependence of cisplatin cytotoxicity on cdk2 activity was also demonstrated because 1) cisplatin caused a marked increase in cdk2 activity, which was prevented by the p21 expression adenovirus, and 2) a cdk2 dominant-negative adenovirus also protected cells from cisplatin-induced apoptosis. Thus the data suggest that the mechanism of p21 protection is by direct inhibition of cdk2 activity and that cisplatin-induced apoptosis is caused by a cdk2-dependent pathway.
机译:p21细胞周期蛋白依赖性激酶(cdk)抑制剂可在体内和体外保护细胞免受顺铂的细胞毒性。但是,保护机制尚不清楚。已知单独的p21结构域可与几种具有促凋亡功能的蛋白质相互作用。为了研究p21的保护机制,我们构建了编码p21不同结构域的腺病毒。我们能够将保护活性定位到包含细胞周期蛋白-cdk相互作用部分的54个氨基酸的区域。 p21的其他蛋白质结合域,包括NH2末端procaspase-3相互作用区域和含有增殖细胞核抗原结合域和核定位信号的COOH末端区域,对顺铂的细胞毒性几乎没有保护作用。还证实了顺铂对cdk2活性的依赖性,因为1)顺铂引起cdk2活性显着增加,这被p21表达腺病毒所阻止; 2)cdk2显性阴性的腺病毒也保护细胞免受顺铂诱导的细胞凋亡。因此,数据表明p21保护的机制是通过直接抑制cdk2活性,而顺铂诱导的凋亡是由cdk2依赖性途径引起的。

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