DNA Damage Responses in Cells Exposed to Sulphur Mustard

Overview

Journal Toxicol Lett

Publisher Elsevier

Specialty Toxicology

Date 2011 Nov 29

PMID 22119920

Citations 16

Authors

Paul A Jowsey

Faith M Williams

Peter G Blain

Affiliations

Soon will be listed here.

Abstract

Sulphur mustard (SM) is a blistering agent that causes debilitating damage to the skin, eyes and respiratory system. In cases of severe exposure, immunodepletion can occur as well as death, due to secondary infections. The toxicity of SM is thought to be mediated in part by the alkylation of nucleic acids and proteins, although the exact mechanisms are not clear. In addition, although the first known use of SM was in military conflict nearly 100 years ago, there are still no effective treatments or preventative measures. In order to develop treatments it is necessary to have a detailed understanding of the cellular biochemical changes induced by SM as well as information on the mechanisms that cells employ to protect against SM toxicity. We have previously demonstrated that the homologous recombination (HR) DNA repair pathway promotes cell survival after SM. This study investigated the role of other DNA repair pathways in the cellular response to SM, specifically base excision repair (BER), nucleotide excision repair (NER) and non-homologous end joining (NHEJ) as well as studying the activation and regulation of DNA damage signalling pathways. Our data confirmed that HR is the major repair pathway protecting against acute SM toxicity, with NER and NHEJ also contributing to cell survival. In addition, this study demonstrated the dose- and time-dependent activation of DNA damage signalling pathways after SM in human TK6 lymphoblastoid cells, in particular the phosphorylation of CHK1, CHK2 and p53. These phosphorylation events were orchestrated by a combination of the ATM and ATR protein kinases.

Citing Articles

Metabolomics Analysis of Rabbit Plasma after Ocular Exposure to Vapors of Sulfur Mustard.

Bouhlel J, Caffin F, Gros-Desormeaux F, Douki T, Benoist J, Castelli F Metabolites. 2024; 14(7).

PMID: 39057672 PMC: 11279318. DOI: 10.3390/metabo14070349.

Treatment of Sulfur Mustard Corneal Injury by Augmenting the DNA Damage Response (DDR): A Novel Approach.

Shalwitz R, Day T, Ruehlmann A, Julio L, Gordon S, Vandeuren A J Pharmacol Exp Ther. 2023; 388(2):526-535.

PMID: 37977813 PMC: 10801765. DOI: 10.1124/jpet.123.001686.

Melatonin as Modulator for Sulfur and Nitrogen Mustard-Induced Inflammation, Oxidative Stress and DNA Damage: Molecular Therapeutics.

Ramos E, Gil-Martin E, de Los Rios C, Egea J, Lopez-Munoz F, Pita R Antioxidants (Basel). 2023; 12(2).

PMID: 36829956 PMC: 9952307. DOI: 10.3390/antiox12020397.

Progress towards a standardized model of ocular sulfur mustard injury for therapeutic testing.

McNutt P Exp Eye Res. 2023; 228:109395.

PMID: 36731603 PMC: 9975063. DOI: 10.1016/j.exer.2023.109395.

Nitrogen Mustard Alkylates and Cross-Links p53 in Human Keratinocytes.

Jan Y, Heck D, An Y, Laskin D, Laskin J Chem Res Toxicol. 2022; 35(4):636-650.

PMID: 35312310 PMC: 9491701. DOI: 10.1021/acs.chemrestox.1c00420.