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Chromatid interchanges induced by the DNA cross-linking agent mitomycin C (MMC) are over-represented in human chromosomes containing large heterochromatic regions. We found that nearly all exchange breakpoints of chromosome 9 are located within the paracentromeric heterochromatin and over 70% of exchanges involving chromosome 9 are between its homologues. We provide evidence that the required pairing of chromosome 9 heterochromatic regions occurs in G0/G1 and S-phase cells as a result of an active cellular process initiated upon MMC treatment. By contrast, no pairing was observed for a euchromatic paracentromeric region of the equal-sized chromosome 8. The MMC-induced pairing of chromosome 9 heterochromatin is observed in a subset of cells; its percentage closely mimics the frequency of homologous interchanges found at metaphase. Moreover, the absence of pairing in cells derived from XPF patients correlates with an altered spectrum of MMC-induced exchanges. Together, the data suggest that the heterochromatin-specific pairing following MMC treatment reflects the initiation of DNA cross-link repair and the formation of exchanges.
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JCS ePress
online publication date 29 Mar 2005
doi: 10.1242/jcs.02306
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118/8/1757
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Research Article
Mitomycin C-induced pairing of heterochromatin reflects initiation of DNA repair and chromatid exchange formation
* Author for correspondence (e-mail: l.mullenders{at}lumc.nl)
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C.-R. Sihn, Y.-S. Lee, J.-S. Jeong, K. Park, and S. H. Kim
CANu1, a novel nucleolar protein, accumulated on centromere in response to DNA damage
Genes Cells,
August 1, 2008;
13(8):
787 - 796.
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© The Company of Biologists Ltd 2005