Repair Pathway Choices and Consequences at the Double-Strand Break

DNA double-strand breaks (DSBs) are cytotoxic lesions that threaten genomic integrity. Failure to repair a DSB has deleterious consequences, including genomic instability and cell death. Indeed, misrepair of DSBs can lead to inappropriate end-joining events, which commonly underlie oncogenic transfo...

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Vydáno v:Trends in cell biology Ročník 26; číslo 1; s. 52 - 64
Hlavní autoři: Ceccaldi, Raphael, Rondinelli, Beatrice, D’Andrea, Alan D.
Médium: Journal Article
Jazyk:angličtina
Vydáno: England Elsevier Ltd 01.01.2016
Témata:
alternative end joining
Animals
Cell Survival
DNA Breaks, Double-Stranded
DNA Repair
Genomic Instability
homologous recombination
Humans
Mutation
Pathology
Polθ
synthetic lethality
homologous recombination
DNA repair
Polθ
alternative end joining
synthetic lethality
ISSN:0962-8924, 1879-3088
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Shrnutí:DNA double-strand breaks (DSBs) are cytotoxic lesions that threaten genomic integrity. Failure to repair a DSB has deleterious consequences, including genomic instability and cell death. Indeed, misrepair of DSBs can lead to inappropriate end-joining events, which commonly underlie oncogenic transformation due to chromosomal translocations. Typically, cells employ two main mechanisms to repair DSBs: homologous recombination (HR) and classical nonhomologous end joining (C-NHEJ). In addition, alternative error-prone DSB repair pathways, namely alternative end joining (alt-EJ) and single-strand annealing (SSA), have been recently shown to operate in many different conditions and to contribute to genome rearrangements and oncogenic transformation. Here, we review the mechanisms regulating DSB repair pathway choice, together with the potential interconnections between HR and the annealing-dependent error-prone DSB repair pathways. Of the four known pathways for repairing DNA DSBs, some evolved towards high-fidelity processes (HR and C-NHEJ), while others are intrinsically mutagenic (alt-EJ and SSA). Some repair pathways are end resection-independent (C-NHEJ), while others are end resection-dependent (HR, alt-EJ, and SSA). End resection likely plays a key role in dictating DNA repair pathway choice. Homology-based repair pathways (HR, alt-EJ, and SSA) are competitive and mutually regulated around the RAD51 presynaptic and postsynaptic steps of HR. Error-prone repair pathways can compensate for the loss of HR. Polθ (an alt-EJ polymerase) is upregulated in HR-deficient cancers: loss of the HR and Polθ-mediated alt-EJ pathways is synthetic lethal.
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ISSN:0962-8924
1879-3088
DOI:10.1016/j.tcb.2015.07.009