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    Mol Cell. 2001 Feb;7(2):263-72.

    BRCA2 is required for homology-directed repair of chromosomal breaks.

    Moynahan ME, Pierce AJ, Jasin M.

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    Department of Medicine, Memorial Sloan-Kettering Cancer Center, New York, NY 10021, USA.

    Abstract

    The BRCA2 tumor suppressor has been implicated in the maintenance of chromosomal stability through a function in DNA repair. In this report, we examine human and mouse cell lines containing different BRCA2 mutations for their ability to repair chromosomal breaks by homologous recombination. Using the I-SceI endonuclease to introduce a double-strand break at a specific chromosomal locus, we find that BRCA2 mutant cell lines are recombination deficient, such that homology-directed repair is reduced 6- to >100-fold, depending on the cell line. Thus, BRCA2 is essential for efficient homology-directed repair, presumably in conjunction with the Rad51 recombinase. We propose that impaired homology-directed repair caused by BRCA2 deficiency leads to chromosomal instability and, possibly, tumorigenesis, through lack of repair or misrepair of DNA damage.

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    PMID:
    11239455
    [PubMed - indexed for MEDLINE]

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