Immortalization of epithelial progenitor cells mediated by resveratrol

被引:0
作者
V P Pearce
J Sherrell
Z Lou
L Kopelovich
W E Wright
J W Shay
机构
[1] UNT Health Science Center at Fort Worth,Department of Pharmacology and Neuroscience
[2] University of North Texas,Department of Cell Biology
[3] School of Dentistry,Division of Cancer Prevention
[4] University of Arizona,undefined
[5] UT Southwestern Medical School,undefined
[6] University of North Texas,undefined
[7] National Cancer Institute,undefined
来源
Oncogene | 2008年 / 27卷
关键词
telomerase; p53; progesterone; breast epithelial; aging;
D O I
暂无
中图分类号
学科分类号
摘要
Within the hierarchy of epithelial stem cells, normal progenitor cells may express regulated telomerase during renewal cycles of proliferation and differentiation. Discontinuous telomerase activity may promote increased renewal capacity of progenitor cells, while deregulated/continuous telomerase activity may promote immortalization when differentiation and/or senescent pathways are compromised. In the present work, we show that resveratrol activates, while progesterone inactivates, continuous telomerase activity within 24 h in subpopulations of human Li–Fraumeni syndrome-derived breast epithelial cells. Resveratrol results in immortalization of mixed progenitor cells with mutant p53, but not human epithelial cells with wild type p53. Our results demonstrate the potential for renewing progenitor cells with mutant p53 to immortalize after continuous telomerase expression when exposed to certain environmental compounds. Understanding the effects of telomerase modulators on endogenous telomerase activity in progenitor cells is relevant to the role of immortalization in the initiation and progression of cancer subtypes.
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页码:2365 / 2374
页数:9
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