4.8 Article

Homologous chromosomes make contact at the sites of double-strand breaks in genes in somatic G0/G1-phase human cells

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.1205759109

Keywords

homologous chromosome interaction; homologous recombination

Funding

  1. National Institutes of Health [R01 CA88041, R01 CA148644]
  2. University of Pittsburgh Cancer Center [P30 CA047904]

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Double-strand DNA breaks (DSBs) are continuously induced in cells by endogenously generated free radicals and exogenous genotoxic agents such as ionizing radiation. DSBs activate the kinase activity in sensor proteins such as ATM and DNA-PK, initiating a complex DNA damage response that coordinates various DNA repair pathways to restore genomic integrity. In this study, we report the unexpected finding that homologous chromosomes contact each other at the sites of DSBs induced by either radiation or the endonuclease I-PpoI in human somatic cells. Contact involves short segments of homologous chromosomes and is centered on a DSB in active genes but does not occur at I-PpoI sites in intergenic DNA. I-PpoI-induced contact between homologous genes is abrogated by the transcriptional inhibitors actinomycin D and alpha-amanitin and requires the kinase activity of ATM but not DNA-PK. Our findings provide documentation of a common transcription-related and ATM kinase-dependent mechanism that induces contact between allelic regions of homologous chromosomes at sites of DSBs in human somatic cells.

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