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BRC-1 acts in the inter-sister pathway of meiotic double-strand break repair

Academic Article
Publication Date:
2008
abstract:
The breast and ovarian cancer susceptibility protein BRCA1 is evolutionarily conserved and functions in DNA double-strand break (DSB) repair through homologous recombination, but its role in meiosis is poorly understood. By using genetic analysis, we investigated the role of the Caenorhabditis elegans BRCA1 orthologue (brc-1) during meiotic prophase. The null mutant in the brc-1 gene is viable, fertile and shows the wild-type complement of six bivalents in most diakinetic nuclei, which is indicative of successful crossover recombination. However,brc-1 mutants show an abnormal increase in apoptosis and RAD-51 foci at pachytene that are abolished by loss of spo-11 function, suggesting a defect in meiosis rather than during premeiotic DNA replication. In genetic backgrounds in which chiasma formation is abrogated, such as him-14/MSH4 and syp-2, loss of brc-1 leads to chromosome fragmentation suggesting that brc-1 is dispensable for crossing over but essential for DSB repair through inter-sister recombination.
Iris type:
01.01 Articolo in rivista
List of contributors:
Adamo, Adele; LA VOLPE, Adriana
Authors of the University:
ADAMO ADELE
Handle:
https://iris.cnr.it/handle/20.500.14243/26326
Published in:
EMBO REPORTS (PRINT)
Journal
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