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首页> 外文期刊>Molecular Carcinogenesis >Telomerase-independent senescence of human immortal cells induced by microcell-mediated chromosome transfer.
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Telomerase-independent senescence of human immortal cells induced by microcell-mediated chromosome transfer.

机译:微细胞介导的染色体转移诱导人类永生细胞的端粒酶非依赖性衰老。

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Maintenance of telomeres, commonly through expression of telomerase activity, is necessary but may not be sufficient for human cells to escape from the cellular senescence program and become immortal. We report here that human tumor cells could undergo cellular senescence in the presence of telomerase activity when a specific normal human chromosome was introduced via microcell-mediated chromosome transfer. The cell models studied include SiHa (uterine cervical carcinoma cells expressing E6 and E7 oncoproteins of human papillomavirus type 16) with a transferred chromosome 2, CC1 (choriocarcinoma cells expressing an amino-terminally truncated p53 protein) with a transferred chromosome 7, and JTC-32 (bladder carcinoma cells) with a transferred chromosome 11. The microcell hybrids with the indicated chromosomes ceased to divide after five to 10 population doublings and showed senescence-associated beta-galactosidase activity but still expressed the genes encoding three components of human telomerase, consistent with the retention of telomerase activity. These results are evidence for barriers to human cell immortalization, which involve activation of unidentified senescence-inducing genes that function independently of inactivation of telomerase.
机译:通常通过端粒酶活性的表达来维持端粒是必要的,但可能不足以使人细胞摆脱细胞衰老程序而变得永生。我们在这里报告,当通过微细胞介导的染色体转移引入特定的正常人类染色体时,人类肿瘤细胞可能在端粒酶活性存在下经历细胞衰老。研究的细胞模型包括具有转移的2号染色体的SiHa(表达16型人乳头瘤病毒E6和E7癌蛋白的子宫宫颈癌细胞),具有转移的7号染色体的CC1(表达氨基末端截短的p53蛋白的绒毛膜癌细胞)和JTC- 32个(膀胱癌细胞),具有11条转移的染色体。具有指定染色体的微细胞杂种在5到10个种群倍增后停止分裂,并显示出与衰老相关的β-半乳糖苷酶活性,但仍表达编码人类端粒酶三个成分的基因,一致保留端粒酶活性。这些结果证明了人类细胞永生化的障碍,其中涉及未鉴定的衰老诱导基因的激活,这些基因的独立于端粒酶的失活而起作用。

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