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Target Concepts:
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Query: UMLS:C0344329 (
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28,634
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
ALC1
(amplified in liver cancer 1), an SNF2 superfamily chromatin-remodeling factor also known as CHD1L (chromodomain helicase/ATPase DNA binding protein 1-like), is implicated in base-excision repair, where PARP (Poly(ADP-ribose) polymerase) mediated Poly(ADP-ribose) signaling facilitates the recruitment of this protein to damage sites. We here demonstrate the critical role played by
ALC1
in the regulation of replication-fork progression in cleaved template strands. To analyze the role played by
ALC1
as well as its functional relationship with PARP1, we generated
ALC1
-/-, PARP1-/-, and
ALC1
-/-/PARP1-/- cells from chicken DT40 cells. We then exposed these cells to camptothecin (CPT), a topoisomerase I poison that generates single-strand breaks and causes the
collapse
of replication forks. The
ALC1
-/- and PARP1-/- cells exhibited both higher sensitivity to CPT and an increased number of chromosome aberrations, compared with wild-type cells. Moreover, phenotypes were very similar across all three mutants, indicating that the role played by
ALC1
in CPT tolerance is dependent upon the PARP pathway. Remarkably, inactivation of
ALC1
resulted in a failure to slow replication-fork progression after CPT exposure, indicating that
ALC1
regulates replication-fork progression at DNA-damage sites. We disrupted ATPase activity by inserting the E165Q mutation into the
ALC1
gene, and found that the resulting
ALC1
-/E165Q cells displayed a CPT sensitivity indistinguishable from that of the null-mutant cells. This observation suggests that
ALC1
contributes to cellular tolerance to CPT, possibly as a chromatin remodeler. This idea is supported by the fact that CPT exposure induced chromatin relaxation in the vicinity of newly synthesized DNA in wild-type but not in
ALC1
-/- cells. This implies a previously unappreciated role for
ALC1
in DNA replication, in which
ALC1
may regulate replication-fork slowing at CPT-induced DNA-damage sites.
...
PMID:Chromatin remodeler ALC1 prevents replication-fork collapse by slowing fork progression. 2940 41
