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Publication : The absence of p53 accelerates atherosclerosis by increasing cell proliferation in vivo.

First Author  Guevara NV Year  1999
Journal  Nat Med Volume  5
Issue  3 Pages  335-9
PubMed ID  10086392 Mgi Jnum  J:53309
Mgi Id  MGI:1332283 Doi  10.1038/6585
Citation  Guevara NV, et al. (1999) The absence of p53 accelerates atherosclerosis by increasing cell proliferation in vivo. Nat Med 5(3):335-9
abstractText  The tumor suppressor protein p53 is an essential molecule in cell proliferation and programmed cell death (apoptosis), and has been postulated to play a principal part in the development of atherosclerosis. We have examined the effect of p53 inactivation on atherogenesis in apoE-knockout mice, an animal model for atherosclerosis. We found that, compared with p53+/+/apoE-/- mice, p53-/-/apoE-/- mice developed considerably accelerated aortic atherosclerosis in the presence of a similar serum cholesterol in response to a high-fat diet. Furthermore, the atherosclerotic lesions in p53-/-/apoE-/- mice had a significant (approximately 280%) increase in cell proliferation rate and an insignificant (approximately 180%) increase in apoptosis compared with those in p53+/+/apoE-/- mice. Our observations indicate that the role of p53 in atherosclerotic lesion development might be associated with its function in cell replication control, and that p53-independent mechanisms can mediate the apoptotic response in atherosclerosis.
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