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Article
Revisiting p53 for Cancer-Specific Chemo- and Radiotherapy: Ten Years after
Cell Cycle
  • Jason M. Beckta
  • Syed Farhan Ahmad
  • Hu Yang, Missouri University of Science and Technology
  • Kristoffer Valerie
Abstract

Despite intense studies, highly effective therapeutic strategies against cancer have not yet been fully exploited, because few true cancer-specific targets have been identified. Most modalities, perhaps with the exception of radiation therapy, target proliferating cells, which are also abundant in normal tissues. Thus, most current cancer treatments have significant side effects. More than 10 years ago, the tumor suppressor p53 was first explored as a cancer-specific target. At the time, the approach was to introduce a normal p53 gene into mutant p53 (mp53) tumor cells to induce cell cycle arrest and apoptosis. However, this strategy did not hold up and mostly failed in subsequent clinical studies. Recent research developments have now returned p53 to the limelight. Several studies have reported that mutant or null p53 tumor cells undergo apoptosis more easily than genetically matched, normal p53 counterparts when inhibiting a specific stress kinase in combination with standard chemotherapy or when exposed to an ataxia-telangiectasia mutated (ATM) kinase inhibitor and radiation, thus achieving true cancer specificity in animal tumor models. This short review highlights several of these recent studies, discusses possible mechanism(s) for mp53-mediated "synthetic lethality", and the implications for cancer therapy.

Department(s)
Chemical and Biochemical Engineering
Keywords and Phrases
  • ATM,
  • DNA damage response,
  • DNA repair,
  • MAPKAP kinase 2,
  • p38
Document Type
Article - Journal
Document Version
Citation
File Type
text
Language(s)
English
Rights
© 2014 Landes Bioscience, All rights reserved.
Publication Date
3-1-2014
Publication Date
01 Mar 2014
PubMed ID
24526114
Citation Information
Jason M. Beckta, Syed Farhan Ahmad, Hu Yang and Kristoffer Valerie. "Revisiting p53 for Cancer-Specific Chemo- and Radiotherapy: Ten Years after" Cell Cycle Vol. 13 Iss. 5 (2014) p. 710 - 713 ISSN: 1538-4101; 1551-4005
Available at: http://works.bepress.com/hu-yang/58/