期刊
EXPERIMENTAL CELL RESEARCH
卷 298, 期 1, 页码 17-27出版社
ELSEVIER INC
DOI: 10.1016/j.yexcr.2004.04.004
关键词
chemotherapy; human fibroblasts; oxidative DNA damage; replicative senescence; stress-induced senescence
资金
- NIA NIH HHS [AG09909, AG17242, AG00266] Funding Source: Medline
Telomerase inhibition may be a novel anti-cancer strategy that can be used in combination with conventional therapies, such as DNA damaging agents. There are conflicting reports as to whether and to what extent telomerase and telomere length influence the sensitivity of cells to genotoxins. To understand the relationship between telomere length, telomerase expression, and sensitivity to genotoxic stress, we expressed the catalytic subunit of telomerase, hTERT, in human fibroblasts having different telomere lengths. We show that telomerase confers resistance to ionizing radiation, bleomycin, hydrogen peroxide, and etoposide only in cells with short, presumably near-dysfunctional, telomeres. This resistance depended on the ability of telomerase to elongate the short telomeres, and telomerase did not protect cells with long telomeres. Interestingly, although long telomeres had no effect on sensitivity to etoposide and bleomycin, they exacerbated sensitivity to hydrogen peroxide, supporting the idea that, compared to other types of DNA damage, telomeres are particularly vulnerable to oxidative damage. Our findings identify a mechanism and conditions under which telomerase and telomeres affect the response of human cells to genotoxic agents and may have important implications for anti-cancer interventions. (C) 2004 Elsevier Inc. All rights reserved.
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