Abstract

The limited proliferative ability of normal animal cells in culture is widely accepted as a manifestation of aging at the cellular level. Most of the investigations of this phenomenon have been devoted to the study of intracellular changes that occur during in vitro aging. However, it is likely that an understanding of the mechanisms leading to the inevitable and essentially irreversable loss of proliferative ability in normal cells will have significance for a large number of biological problems, including the processes of neoplasia and abnormal development. Recent experimental evidence from cell hybridization and cell reconstruction experiments has led to the idea that after a period of active growth in culture normal cells produce a specific substance(s) that prevents DNA synthesis and cell division, thereby resulting in what has been commonly called cellular senescence. We have further found that human diploid fibroblasts held in a nondividing state (quiescent cells) produce an inhibitory substance(s) similar to that produced by senescent cells. Proteins that block the initiation of DNA synthesis can be extracted from the membranes of these cells and, when poly(A)+ mRNA from senescent cells is microinjected into young cells, the initiation of DNA synthesis is blocked. The project proposed in this application will be to identify, isolate and characterize the protein products responsible for the inhibitory activity of senescent and quiescent cells and the mRNAs and genomic DNA coding for them. We will then begin to study the control of expression of the genes and the relationship of in vitro cellular senescence to actual in vivo cellular aging. Monoclonal antibodies to the senescence and quiescence factors will be prepared and used in immunocytochemical studies to determine the cellular localization of the factors in aging human diploid fibroblasts, vascular endothelial cells, and keratinocytes. cDNA probes will be prepared to the mRNA coding for the senescence and quiescence factors. These will be used to perform preliminary structural studies on the senescence factor gene and to study the regulation of senescence and quiescence factors.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
5R01AG004749-05
Application #
3115323
Study Section
Cellular Biology and Physiology Subcommittee 1 (CBY)
Project Start
1983-09-01
Project End
1989-06-30
Budget Start
1987-09-01
Budget End
1989-06-30
Support Year
5
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

Name
Baylor College of Medicine
Department
Type
Schools of Medicine
DUNS #
074615394
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Krause, Neal (2004) Religion, aging, and health: exploring new frontiers in medical care. South Med J 97:1215-22
Smith, J R; Pereira-Smith, O M (1990) Genetic and molecular studies of cellular immortalization. Adv Cancer Res 54:63-77
Porter, M B; Pereira-Smith, O M; Smith, J R (1990) Novel monoclonal antibodies identify antigenic determinants unique to cellular senescence. J Cell Physiol 142:425-33
Porter, M B; Smith, J R (1990) Role of endogenous proteins as negative growth modulators during in vitro cellular aging of human diploid fibroblasts. Annu Rev Gerontol Geriatr 10:53-70
Smith, J R; Pereira-Smith, O M (1989) Altered gene expression during cellular aging. Genome 31:386-9
West, M D; Pereira-Smith, O M; Smith, J R (1989) Replicative senescence of human skin fibroblasts correlates with a loss of regulation and overexpression of collagenase activity. Exp Cell Res 184:138-47
McClung, J K; Danner, D B; Stewart, D A et al. (1989) Isolation of a cDNA that hybrid selects antiproliferative mRNA from rat liver. Biochem Biophys Res Commun 164:1316-22
Smith, J R; Pereira-Smith, O M (1989) Further studies on the genetic and biochemical basis of cellular senescence. Exp Gerontol 24:377-81
Pereira-Smith, O M; Smith, J R (1988) Genetic analysis of indefinite division in human cells: identification of four complementation groups. Proc Natl Acad Sci U S A 85:6042-6
Spiering, A L; Smith, J R; Pereira-Smith, O M (1988) A potent DNA synthesis inhibitor expressed by the immortal cell line SUSM-1. Exp Cell Res 179:159-67

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