The factors that cause cancer, a major health problem of the elderly, are still elusive. We are addressing this problem by studying molecular mechanisms of aging and cancer using cellular models. We have shown that, by means of microcell-mediated chromosome transfer, normal cells have telomerase-dependent and telomerase-independent pathways for cellular senescence, which both serve as a tumor suppressive mechanism in humans. The senescence gene on chromosome 3p21 functions through the transcriptional repression of the hTERT gene (encoding the telomerase catalytic subunit). We have identified a cis-element within the hTERT promoter region responsible for the repression, and a protein factor binding to this element is currently under investigation. A senescence gene on chromosome 1q42, which acts independently of telomerase regulation, is also to be cloned by the positional and functional cloning methods. To understand a link between cellular aging and organismal aging, we study SIRTs, human homologs of the yeast/worm longevity gene Sir-2 encoding a protein deacetylase, and Hic-5, a LIM domain protein that may play a role in commitment to cellular senescence. In addition to analyses of these specific genes, our projects include: aging-associated changes in global gene expression, which may involve chromatin structure regulated by histone modifications; and a role of DNA damage (e.g., double strand breaks and oxidative damage) in aging.

Agency
National Institute of Health (NIH)
Institute
Division of Basic Sciences - NCI (NCI)
Type
Intramural Research (Z01)
Project #
1Z01BC010417-03
Application #
6763831
Study Section
(LBC)
Project Start
Project End
Budget Start
Budget End
Support Year
3
Fiscal Year
2002
Total Cost
Indirect Cost
Name
Basic Sciences
Department
Type
DUNS #
City
State
Country
United States
Zip Code
Sedelnikova, Olga A; Horikawa, Izumi; Zimonjic, Drazen B et al. (2004) Senescing human cells and ageing mice accumulate DNA lesions with unrepairable double-strand breaks. Nat Cell Biol 6:168-70
Li, Shuanfang; Hursting, Stephen D; Davis, Barbara J et al. (2003) Environmental exposure, DNA methylation, and gene regulation: lessons from diethylstilbesterol-induced cancers. Ann N Y Acad Sci 983:161-9
Li, Shuanfang; Hansman, Roberta; Newbold, Retha et al. (2003) Neonatal diethylstilbestrol exposure induces persistent elevation of c-fos expression and hypomethylation in its exon-4 in mouse uterus. Mol Carcinog 38:78-84
Xiao, Xiaodong; Athanasiou, Meropi; Sidorov, Igor A et al. (2003) Role of Ets/Id proteins for telomerase regulation in human cancer cells. Exp Mol Pathol 75:238-47
Tsutsui, Takeki; Kumakura, Shin-Ichi; Tamura, Yukiko et al. (2003) Immortal, telomerase-negative cell lines derived from a Li-Fraumeni syndrome patient exhibit telomere length variability and chromosomal and minisatellite instabilities. Carcinogenesis 24:953-65
Burroughs, Kevin D; Oh, Jennifer; Barrett, J Carl et al. (2003) Phosphatidylinositol 3-kinase and mek1/2 are necessary for insulin-like growth factor-I-induced vascular endothelial growth factor synthesis in prostate epithelial cells: a role for hypoxia-inducible factor-1? Mol Cancer Res 1:312-22
Tsutsui, Takeki; Tamura, Yukiko; Yagi, Eiichi et al. (2003) Cell-transforming activity and mutagenicity of 5 phytoestrogens in cultured mammalian cells. Int J Cancer 105:312-20
Horikawa, Izumi; Barrett, J Carl (2003) Transcriptional regulation of the telomerase hTERT gene as a target for cellular and viral oncogenic mechanisms. Carcinogenesis 24:1167-76
Shigeeda, Nobumasa; Uchida, Minoru; Barrett, J Carl et al. (2003) Candidate chromosomal regions for genes involved in activation of alternative lengthening of telomeres in human immortal cell lines. Exp Gerontol 38:641-51
Kenney, Nicholas J; Bowman, Arthur; Korach, Kenneth S et al. (2003) Effect of exogenous epidermal-like growth factors on mammary gland development and differentiation in the estrogen receptor-alpha knockout (ERKO) mouse. Breast Cancer Res Treat 79:161-73

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