Replicative senescence: implications for in vivo aging and tumor suppression

JR Smith, OM Pereira-Smith - Science, 1996 - science.org
JR Smith, OM Pereira-Smith
Science, 1996science.org
Normal cells have limited proliferative potential in culture, a fact that has been the basis of
their use as a model for replicative senescence for many years. Recent molecular analyses
have identified numerous changes in gene expression that occur as cells become
senescent, and the results indicate that multiple levels of control contribute to the irreversible
growth arrest. These include repression of growth stimulatory genes, overexpression of
growth inhibitory genes, and interference with downstream pathways. Studies with cell types …
Normal cells have limited proliferative potential in culture, a fact that has been the basis of their use as a model for replicative senescence for many years. Recent molecular analyses have identified numerous changes in gene expression that occur as cells become senescent, and the results indicate that multiple levels of control contribute to the irreversible growth arrest. These include repression of growth stimulatory genes, overexpression of growth inhibitory genes, and interference with downstream pathways. Studies with cell types other than fibroblasts will better define the role of cell senescence in the aging process and in tumorigenesis.
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