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外文期刊>The biochemical journal
>Apoptosis or senescence-like growth arrest: influence of cell-cycle position, p53, p21 and bax in H2O2 response of normal human fibroblasts
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Apoptosis or senescence-like growth arrest: influence of cell-cycle position, p53, p21 and bax in H2O2 response of normal human fibroblasts
pEarly-passage human diploid fibroblasts (HDFs) undergo senescence-like growth arrest in response to sublethal concentrations of Hsub2/subOsub2/sub [Chen and Ames (1994) Proc. Natl. Acad. Sci. U.S.A. 95, 4130-4134]. We determine here whether Hsub2/subOsub2/sub can cause apoptosis in HDFs and the molecular changes that differ between apoptosis and senescence-like growth arrest. When exponentially growing early-passage IMR-90 cells were treated for 2 h with 50-200 iμ/iM (or 0.25-1 pmol/cell) Hsub2/subOsub2/sub, a fraction of cells detached at 16-32 h after the treatment. The cells remaining attached were growth-arrested and developed features of senescence in 1 week. The detached cells showed caspase-3 activation and typical morphological changes associated with apoptosis. Caspase-3 activation was Hsub2/subOsub2/sub dose-dependent and preceded nuclear condensation or plasma membrane leakage. Apoptotic cells were mainly distributed in the S-phase of the cell cycle, while growth-arrested cells exhibited predominantly G1- and G2/M-phase distributions. Hsub2/subOsub2/sub pretreatment induced G1 arrest and prohibited induction of apoptosis by a subsequent Hsub2/subOsub2/sub challenge. The p53 protein showed an average 6.1-fold elevation in apoptotic cells and a 3.5-fold elevation in growth-arrested cells. Reduction of p53 levels with human papillomavirus E6 protein prohibited the activation of caspase-3 and decreased the proportion of apoptotic cells. Growth-arrested cells had elevated p21, while p21 was absent in apoptotic cells. Bcl-2 was elevated in both growth-arrested and apoptotic cells. Finally, although the overall level of bax did not change in growth-arrested or apoptotic cells, the solubility of bax protein increased in apoptotic cells. Our data suggest that in contrast with growth-arrested cells, apoptotic cells show an S-phase cell cycle distribution, a higher degree of p53 elevation, an absence of p21 protein and increased solubility of bax protein./p
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机译:>早期人类二倍体成纤维细胞(HDFs)响应于亚致死浓度的H 2 O 2 经历衰老样生长停滞[Chen and Ames(1994)Proc。 。 Natl。学院科学U.S.A. 95,4130-4134]。我们在这里确定H 2 O 2 是否会导致HDFs凋亡以及凋亡和衰老样生长停滞之间的分子变化。当指数增长的早期传代IMR-90细胞用50-200μiM(或0.25-1 pmol /细胞)H 2 O 处理2 h 2 ,部分细胞在处理后16-32 h脱落。保留附着的细胞在1周内被阻止生长并形成衰老特征。分离的细胞显示出caspase-3活化和与凋亡相关的典型形态变化。 Caspase-3激活是H 2 O 2 剂量依赖性的,并先于核浓缩或质膜泄漏。凋亡细胞主要分布在细胞周期的S期,而生长停滞的细胞则主要分布在G1和G2 / M期。 H 2 O 2 预处理可诱导G1阻滞,并阻止随后的H 2 O 2 攻击诱导细胞凋亡。 p53蛋白在凋亡细胞中平均升高6.1倍,在生长停滞细胞中升高3.5倍。人乳头瘤病毒E6蛋白降低p53水平阻止了caspase-3的活化,并降低了凋亡细胞的比例。生长停滞的细胞具有升高的p21,而凋亡细胞中不存在p21。 Bcl-2在生长停滞和凋亡细胞中均升高。最后,尽管在生长停滞或凋亡的细胞中bax的总体水平没有变化,但bax蛋白在凋亡细胞中的溶解度却增加了。我们的数据表明,与生长停滞的细胞相比,凋亡细胞表现出S期细胞周期分布,p53升高程度更高,p21蛋白不存在以及bax蛋白的溶解度增加。
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