| Literature DB >> 28017613 |
Kristopher A Sarosiek1, Cameron Fraser2, Nathiya Muthalagu3, Patrick D Bhola1, Weiting Chang4, Samuel K McBrayer1, Adam Cantlon4, Sudeshna Fisch4, Gail Golomb-Mello5, Jeremy A Ryan1, Jing Deng1, Brian Jian6, Chris Corbett7, Marti Goldenberg7, Joseph R Madsen8, Ronglih Liao4, Dominic Walsh4, John Sedivy5, Daniel J Murphy9, Daniel Ruben Carrasco1, Shenandoah Robinson8, Javid Moslehi10, Anthony Letai11.
Abstract
It is not understood why healthy tissues can exhibit varying levels of sensitivity to the same toxic stimuli. Using BH3 profiling, we find that mitochondria of many adult somatic tissues, including brain, heart, and kidneys, are profoundly refractory to pro-apoptotic signaling, leading to cellular resistance to cytotoxic chemotherapies and ionizing radiation. In contrast, mitochondria from these tissues in young mice and humans are primed for apoptosis, predisposing them to undergo cell death in response to genotoxic damage. While expression of the apoptotic protein machinery is nearly absent by adulthood, in young tissues its expression is driven by c-Myc, linking developmental growth to cell death. These differences may explain why pediatric cancer patients have a higher risk of developing treatment-associated toxicities.Entities:
Keywords: apoptosis; c-Myc; cardiotoxicity; cell death regulation; chemosensitivity; neurotoxicity; pediatric cancer; radiosensitivity; side effects of chemotherapy; side effects of radiation therapy
Mesh:
Substances:
Year: 2016 PMID: 28017613 PMCID: PMC5363285 DOI: 10.1016/j.ccell.2016.11.011
Source DB: PubMed Journal: Cancer Cell ISSN: 1535-6108 Impact factor: 31.743