Distinct DNA repair mechanisms prevent formaldehyde toxicity during development, reproduction and aging

Abstract Formaldehyde (FA) is a recognized environmental and metabolic toxin implicated in cancer development and aging. Inherited mutations in the FA-detoxifying enzymes ADH5 and ALDH2 genes lead to FA overload in the severe multisystem AMeD syndrome. FA accumulation causes genome damage including...

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Bibliographic Details
Published in:Nucleic acids research 2024-08, Vol.52 (14), p.8271-8285
Main Authors: Rieckher, Matthias, Gallrein, Christian, Alquezar-Artieda, Natividad, Bourached-Silva, Nour, Vaddavalli, Pavana Lakshmi, Mares, Devin, Backhaus, Maria, Blindauer, Timon, Greger, Ksenia, Wiesner, Eva, Pontel, Lucas B, Schumacher, Björn
Format: Article
Language:English
Subjects:
Acetylcysteine - pharmacology
Aging - genetics
Aldehyde Dehydrogenase - genetics
Aldehyde Dehydrogenase - metabolism
Aldehyde Oxidoreductases
Animals
Caenorhabditis elegans - drug effects
Caenorhabditis elegans - genetics
Caenorhabditis elegans - growth & development
Caenorhabditis elegans Proteins - genetics
Caenorhabditis elegans Proteins - metabolism
DNA Damage
DNA Repair
Formaldehyde - toxicity
Genome Integrity, Repair and
Humans
Mutation
Reproduction - drug effects
Reproduction - genetics
Transcription, Genetic - drug effects
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Summary:Abstract Formaldehyde (FA) is a recognized environmental and metabolic toxin implicated in cancer development and aging. Inherited mutations in the FA-detoxifying enzymes ADH5 and ALDH2 genes lead to FA overload in the severe multisystem AMeD syndrome. FA accumulation causes genome damage including DNA–protein-, inter- and intra-strand crosslinks and oxidative lesions. However, the influence of distinct DNA repair systems on organismal FA resistance remains elusive. We have here investigated the consequence of a range of DNA repair mutants in a model of endogenous FA overload generated by downregulating the orthologs of human ADH5 and ALDH2 in C. elegans. We have focused on the distinct components of nucleotide excision repair (NER) during developmental growth, reproduction and aging. Our results reveal three distinct modes of repair of FA-induced DNA damage: Transcription-coupled repair (TCR) operating NER-independently during developmental growth or through NER during adulthood, and, in concert with global-genome (GG-) NER, in the germline and early embryonic development. Additionally, we show that the Cockayne syndrome B (CSB) factor is involved in the resolution of FA-induced DNA–protein crosslinks, and that the antioxidant and FA quencher N-acetyl-l-cysteine (NAC) reverses the sensitivity of detoxification and DNA repair defects during development, suggesting a therapeutic intervention to revert FA-pathogenic consequences. Graphical Abstract Graphical Abstract
ISSN:0305-1048
1362-4962
1362-4962
DOI:10.1093/nar/gkae519