Abstract

The hallmark of cellular aging is the failure of senescent cells to enter/complete the S phase of the cell cycle. The cause for such failure may hold the key for our outstanding the molecular basis of cellular aging. Our previous results demonstrated no difference in the levels of c-myc mRNA and ornithine decarboxylase (ODC) mRNA, but a marked reduction of thymidine kinase (TK) gene expression in old IMR_90 cells as compared to that of the young cells. In addition to TK, all other G1/S genes examined, including thymidine synthase, dihydrofolate reductase, PCNA, histones 1, 3, and 4, exhibited marked attenuation of gene expression in senescent cells, suggesting that such an attenuation may represent a global change critically associated with cellular aging. It is likely that the control of these G1/S genes may play a fundamental role in aging. Preliminary studies using transient expression assay suggest that the age-dependent attenuation of TK gene expression is transcriptionally regulated. Gel mobility shift assay using a 67-bp fragment containing an inverted CCAAT box in the TK promoter suggested that a nuclear trans-acting factor named as CBP-II (CCAAT-Binding Protein II) may be involved in this regulation. CBP-II binding is serum- inducible and age-dependent, prominent in young but not in old IMR-90 cells. CBP-II also appears to be labile, with a half-lifeless than 30 minutes. The main objective of this proposal is to study the role of CBP-II, a newly found trans-acting factor, in the regulation of TK gene. To achieve this goal, we plan to characterize and purify CBP-II using sequence-specific DNA affinity chromatography and gel mobility shift assay. We will also use various screening procedures, including the use of recognition site probes (e.g. the 67-bp) to obtain the CBP-II cDNA. We will use both sense and antisense CBP-II cDNA to construct recombinant plasmids with appropriate DNA expression vectors. Stably transfected IMR_90 cells using these plasmids will allow us to evaluate the role of CBP-II in regulating TK gene expression. In addition, these constructs may also enable us to investigate whether CBP-II is involved in regulating other G1/S genes. Trans-acting factor CBP-II may be critically involved in the regulation of TK gene during aging. The proposed study should yield a deeper understanding of the mechanism of TK gene regulation. It is possible that trans-acting factors such as CBP-II may play a key role in regulating G1/S genes during cellular aging.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
2R01AG003578-07
Application #
3114794
Study Section
Molecular Cytology Study Section (CTY)
Project Start
1982-09-29
Project End
1997-06-30
Budget Start
1992-07-02
Budget End
1993-06-30
Support Year
7
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
Rutgers University
Department
Type
Schools of Arts and Sciences
DUNS #
038633251
City
New Brunswick
State
NJ
Country
United States
Zip Code
08901

  Publications

Lu, J; Park, J H; Liu, A Y et al. (2000) Activation of heat shock factor 1 by hyperosmotic or hypo-osmotic stress is drastically attenuated in normal human fibroblasts during senescence. J Cell Physiol 184:183-90
Matuoka, K; Chen, K Y (2000) Possible role of subunit A of nuclear factor Y (NF-YA) in normal human diploid fibroblasts during senescence. Biogerontology 1:261-71
Matuoka, K; Yu Chen, K (1999) Nuclear factor Y (NF-Y) and cellular senescence. Exp Cell Res 253:365-71
Chen, K Y (1997) Transcription factors and the down-regulation of G1/S boundary genes in human diploid fibroblasts during senescence. Front Biosci 2:d417-26
Chen, Z P; Chen, K Y (1997) Dramatic attenuation of hypusine formation on eukaryotic initiation factor 5A during senescence of IMR-90 human diploid fibroblasts. J Cell Physiol 170:248-54
Caruccio, L; Bae, S; Liu, A Y et al. (1997) The heat-shock transcription factor HSF1 is rapidly activated by either hyper- or hypo-osmotic stress in mammalian cells. Biochem J 327 ( Pt 2):341-7
Good, L F; Chen, K Y (1996) Cell cycle- and age-dependent transcriptional regulation of human thymidine kinase gene: the role of NF-Y in the CBP/tk binding complex. Biol Signals 5:163-9
Pang, J H; Good, L F; Chen, K Y (1996) The age-dependent binding of CBP/tk, a CCAAT binding protein, is deregulated in transformed and immortalized mammalian cells but absent in premature aging cells. Exp Gerontol 31:97-109
Good, L; Dimri, G P; Campisi, J et al. (1996) Regulation of dihydrofolate reductase gene expression and E2F components in human diploid fibroblasts during growth and senescence. J Cell Physiol 168:580-8
Huang, L E; Caruccio, L; Liu, A Y et al. (1995) Rapid activation of the heat shock transcription factor, HSF1, by hypo-osmotic stress in mammalian cells. Biochem J 307 ( Pt 2):347-52

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