4.4 Article

Telomerase activity in response to mild oxidative stress

Journal

CELL BIOLOGY INTERNATIONAL
Volume 36, Issue 4, Pages 409-413

Publisher

WILEY
DOI: 10.1042/CBI20110308

Keywords

bcl-2; BCL-2; chemotherapeutic drugs; oxidative stress; telomerase

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Funding

  1. CONACYT [CB-2006-1-59659]

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We have analysed telomerase activity to determine whether it can be modified when BCL-2 is endogenously overexpressed in response to a mild oxidative stress treatment as part of a survival mechanism, in contrast with an exogenous bcl-2 overexpression due to a retroviral infection. Endogenous bcl-2overexpression was induced after a low oxidative insult of H2O2 in mice primary lung fibroblasts and L929 cell, whereas bcl-2 exogenous overexpression was performed using a retroviral infection in L929 cells. Telomerase activity was quantified in Bcl-2overexpressing cells by the TRAP assay. When the cells were treated with different H2O2 concentrations, only those exposed to 50 mu M showed increased telomerase activity. This correlates with BCL-2 expression as part of the endogenous response to mild oxidative stress. Oxidative stress generated during the toxic mechanism of chemotherapeutic drugs might induce BCL-2 increment, enhancing telomerase activity and reactivating the oncogenic process. Clinical trials should take into consideration the possibility of telomerase activation following increased BCL-2 expression when treating patients with ROS (reactive oxygen species) generation by anti-cancer drugs.

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