Homology-mediated end-capping as a primary step of sister chromatid fusion in the breakage-fusion-bridge cycles

نویسندگان

  • Michael Marotta
  • Xiongfong Chen
  • Takaaki Watanabe
  • Pieter W. Faber
  • Scott J. Diede
  • Stephen Tapscott
  • Raymond Tubbs
  • Anna Kondratova
  • Robert Stephens
  • Hisashi Tanaka
چکیده

Breakage-fusion-bridge (BFB) cycle is a series of chromosome breaks and duplications that could lead to the increased copy number of a genomic segment (gene amplification). A critical step of BFB cycles leading to gene amplification is a palindromic fusion of sister chromatids following the rupture of a dicentric chromosome during mitosis. It is currently unknown how sister chromatid fusion is produced from a mitotic break. To delineate the process, we took an integrated genomic, cytogenetic and molecular approach for the recurrent MCL1 amplicon at chromosome 1 in human tumor cells. A newly developed next-generation sequencing-based approach identified a cluster of palindromic fusions within the amplicon at ∼50-kb intervals, indicating a series of breaks and fusions by BFB cycles. The physical location of the amplicon (at the end of a broken chromosome) further indicated BFB cycles as underlying processes. Three palindromic fusions were mediated by the homologies between two nearby inverted Alu repeats, whereas the other two fusions exhibited microhomology-mediated events. Such breakpoint sequences indicate that homology-mediated fold-back capping of broken ends followed by DNA replication is an underlying mechanism of sister chromatid fusion. Our results elucidate nucleotide-level events during BFB cycles and end processing for naturally occurring mitotic breaks.

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عنوان ژورنال:

دوره 41  شماره 

صفحات  -

تاریخ انتشار 2013