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Double-strand DNA breaks recruit the centromeric histone CENP-A.


ABSTRACT: The histone H3 variant CENP-A is required for epigenetic specification of centromere identity through a loading mechanism independent of DNA sequence. Using multiphoton absorption and DNA cleavage at unique sites by I-SceI endonuclease, we demonstrate that CENP-A is rapidly recruited to double-strand breaks in DNA, along with three components (CENP-N, CENP-T, and CENP-U) associated with CENP-A at centromeres. The centromere-targeting domain of CENP-A is both necessary and sufficient for recruitment to double-strand breaks. CENP-A accumulation at DNA breaks is enhanced by active non-homologous end-joining but does not require DNA-PKcs or Ligase IV, and is independent of H2AX. Thus, induction of a double-strand break is sufficient to recruit CENP-A in human and mouse cells. Finally, since cell survival after radiation-induced DNA damage correlates with CENP-A expression level, we propose that CENP-A may have a function in DNA repair.

SUBMITTER: Zeitlin SG 

PROVIDER: S-EPMC2747192 | biostudies-literature | 2009 Sep

REPOSITORIES: biostudies-literature

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Double-strand DNA breaks recruit the centromeric histone CENP-A.

Zeitlin Samantha G SG   Baker Norman M NM   Chapados Brian R BR   Soutoglou Evi E   Wang Jean Y J JY   Berns Michael W MW   Cleveland Don W DW  

Proceedings of the National Academy of Sciences of the United States of America 20090828 37


The histone H3 variant CENP-A is required for epigenetic specification of centromere identity through a loading mechanism independent of DNA sequence. Using multiphoton absorption and DNA cleavage at unique sites by I-SceI endonuclease, we demonstrate that CENP-A is rapidly recruited to double-strand breaks in DNA, along with three components (CENP-N, CENP-T, and CENP-U) associated with CENP-A at centromeres. The centromere-targeting domain of CENP-A is both necessary and sufficient for recruitm  ...[more]

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