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    Mol Cytogenet. 2012 Jan 19;5(1):6.

    A recurrent translocation is mediated by homologous recombination between HERV-H elements.

    Source

    Department of Human Genetics, Emory University School of Medicine, Atlanta, GA, USA. katie.rudd@emory.edu.

    Abstract

    ABSTRACT:

    BACKGROUND:

    Chromosome rearrangements are caused by many mutational mechanisms; of these, recurrent rearrangements can be particularly informative for teasing apart DNA sequence-specific factors. Some recurrent translocations are mediated by homologous recombination between large blocks of segmental duplications on different chromosomes. Here we describe a recurrent unbalanced translocation casued by recombination between shorter homologous regions on chromosomes 4 and 18 in two unrelated children with intellectual disability.

    RESULTS:

    Array CGH resolved the breakpoints of the 6.97-Megabase (Mb) loss of 18q and the 7.30-Mb gain of 4q. Sequencing across the translocation breakpoints revealed that both translocations occurred between 92%-identical human endogenous retrovirus (HERV) elements in the same orientation on chromosomes 4 and 18. In addition, we find sequence variation in the chromosome 4 HERV that makes one allele more like the chromosome 18 HERV.

    CONCLUSIONS:

    Homologous recombination between HERVs on the same chromosome is known to cause chromosome deletions, but this is the first report of interchromosomal HERV-HERV recombination leading to a translocation. It is possible that normal sequence variation in substrates of non-allelic homologous recombination (NAHR) affects the alignment of recombining segments and influences the propensity to chromosome rearrangement.

    PMID:
    22260357
    [PubMed - in process]
    PMCID:
    PMC3292815
    Free PMC Article

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