Induction of CAF-1 expression in response to DNA strand breaks in quiescent human cells

A Nabatiyan, D Szüts, T Krude - Molecular and Cellular Biology, 2006 - Taylor & Francis
A Nabatiyan, D Szüts, T Krude
Molecular and Cellular Biology, 2006Taylor & Francis
Genome stability in eukaryotic cells is maintained through efficient DNA damage repair
pathways, which have to access and utilize chromatin as their natural template. Here we
investigate the role of chromatin assembly factor 1 (CAF-1) and its interacting protein, PCNA,
in the response of quiescent human cells to DNA double-strand breaks (DSBs). The
expression of CAF-1 and PCNA is dramatically induced in quiescent cells upon the
generation of DSBs by the radiomimetic drug bleocin (a bleomycin compound) or by ionizing …
Genome stability in eukaryotic cells is maintained through efficient DNA damage repair pathways, which have to access and utilize chromatin as their natural template. Here we investigate the role of chromatin assembly factor 1 (CAF-1) and its interacting protein, PCNA, in the response of quiescent human cells to DNA double-strand breaks (DSBs). The expression of CAF-1 and PCNA is dramatically induced in quiescent cells upon the generation of DSBs by the radiomimetic drug bleocin (a bleomycin compound) or by ionizing radiation. This induction depends on DNA-PK. CAF-1 and PCNA are recruited to damaged chromatin undergoing DNA repair of single- and double-strand DNA breaks by the base excision repair and nonhomologous end-joining pathways, respectively, in the absence of extensive DNA synthesis. CAF-1 prepared from repair-proficient quiescent cells after induction by bleocin mediates nucleosome assembly in vitro. Depletion of CAF-1 by RNA interference in bleocin-treated quiescent cells in vivo results in a significant loss of cell viability and an accumulation of DSBs. These results support a novel and essential role for CAF-1 in the response of quiescent human cells to DSBs, possibly by reassembling chromatin following repair of DNA strand breaks.
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