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Contributions of DNA repair and damage response pathways to the non-linear genotoxic responses of alkylating agents

期刊

出版社

ELSEVIER SCIENCE BV
DOI: 10.1016/j.mrrev.2015.11.001

关键词

DNA damage; DNA repair; Biological pathways; Low-dose; Dose-response; Points of departure

资金

  1. National Institutes of Health (NIH) [R01-CA079827, U01-ES016045]
  2. NIH [P30-ES002109, CA181959]
  3. Unilever Safety & Environmental Assurance Centre, UK
  4. ExxonMobil Foundation, USA
  5. State of Connecticut [13-SCB-UCHC-06]
  6. [R21-ES019498]

向作者/读者索取更多资源

From a risk assessment perspective, DNA-reactive agents are conventionally assumed to have genotoxic risks at all exposure levels, thus applying a linear extrapolation for low-dose responses. New approaches discussed here, including more diverse and sensitive methods for assessing DNA damage and DNA repair, strongly support the existence of measurable regions where genotoxic responses with increasing doses are insignificant relative to control. Model monofunctional alkylating agents have in vitro and in vivo datasets amenable to determination of points of departure (PoDs) for genotoxic effects. A session at the 2013 Society of Toxicology meeting provided an opportunity to survey the progress in understanding the biological basis of empirically-observed PoDs for DNA alkylating agents. Together with the literature published since, this review discusses cellular pathways activated by endogenous and exogenous alkylation DNA damage. Cells have evolved conserved processes that monitor and counteract a spontaneous steady-state level of DNA damage. The ubiquitous network of DNA repair pathways serves as the first line of defense for clearing of the DNA damage and preventing mutation. Other biological pathways discussed here that are activated by genotoxic stress include post-translational activation of cell cycle networks and transcriptional networks for apoptosis/cell death. The interactions of various DNA repair and DNA damage response pathways provide biological bases for the observed PoD behaviors seen with genotoxic compounds. Thus, after formation of DNA adducts, the activation of cellular pathways can lead to the avoidance of a mutagenic outcome. The understanding of the cellular mechanisms acting within the low-dose region will serve to better characterize risks from exposures to DNA-reactive agents at environmentally-relevant concentrations. (C) 2015 Elsevier B.V. All rights reserved.

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