Pathologies Associated with the p53 Response (original) (raw)

Elena A. Komarova 1
1Department of Cell Stress Biology, Roswell Park Cancer Institute, Buffalo, New York 14263
2Cleveland BioLabs, Inc., Buffalo, New York 14203
Correspondence: andrei.gudkov{at}roswellpark.org

Abstract

Although p53 is a major cancer preventive factor, under certain extreme stress conditions it may induce severe pathologies. Analyses of animal models indicate that p53 is largely responsible for the toxicity of ionizing radiation or DNA damaging drugs contributing to hematopoietic component of acute radiation syndrome and largely determining severe adverse effects of cancer treatment. p53-mediated damage is strictly tissue specific and occurs in tissues prone to p53-dependent apoptosis (e.g., hematopoietic system and hair follicles); on the contrary, p53 can serve as a survival factor in tissues that respond to p53 activation by cell cycle arrest (e.g., endothelium of small intestine). There are multiple experimental indications that p53 contributes to pathogenicity of acute ischemic diseases. Temporary reversible suppression of p53 by small molecules can be an effective and safe approach to reduce severity of p53-associated pathologies.

Footnotes

Editors: Arnold J. Levine and David P. Lane
Additional Perspectives on The p53 Family available at www.cshperspectives.org