APLF (C2orf13) Is a Novel Component of Poly(ADP-Ribose) Signaling in Mammalian Cells

Rulten, Stuart L.; Cortés‐Ledesma, Felipe; Guo, Liandi; Iles, Natasha; Caldecott, Keith W.

doi:10.1128/mcb.02243-07

Cited by 88 publications

(77 citation statements)

References 35 publications

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“…To date, three PAR-binding motifs have been identified in various proteins, including the putative consensus sequence of an eight amino-acid motif 30,31 , the PAR-binding zinc-finger (PBZ) motif 32,33 and the macrodomains [34][35][36] . Despite the universal nature of the poly(ADP-ribosyl)ation of target proteins, and PARP's function in a wide range of cellular activities 21,25 , only a limited number of PAR-binding motifs have been found in several target proteins 20,37 .…”

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confidence: 99%

Poly(ADP-ribose) binding to Chk1 at stalled replication forks is required for S-phase checkpoint activation

et al. 2013

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Damaged replication forks activate poly(ADP-ribose) polymerase 1 (PARP1), which catalyses poly(ADP-ribose) (PAR) formation; however, how PARP1 or poly(ADP-ribosyl)ation is involved in the S-phase checkpoint is unknown. Here we show that PAR, supplied by PARP1, interacts with Chk1 via a novel PAR-binding regulatory (PbR) motif in Chk1, independent of ATR and its activity. iPOND studies reveal that Chk1 associates readily with the unperturbed replication fork and that PAR is required for efficient retention of Chk1 and phosphorylated Chk1 at the fork. A PbR mutation, which disrupts PAR binding, but not the interaction with its partners Claspin or BRCA1, impairs Chk1 and the S-phase checkpoint activation, and mirrors Chk1 knockdown-induced hypersensitivity to fork poisoning. We find that long chains, but not short chains, of PAR stimulate Chk1 kinase activity. Collectively, we disclose a previously unrecognized mechanism of the S-phase checkpoint by PAR metabolism that modulates Chk1 activity at the replication fork.

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confidence: 99%

Poly(ADP-ribose) binding to Chk1 at stalled replication forks is required for S-phase checkpoint activation

et al. 2013

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“…But, a 70% of knockdown of APLF at the protein level failed to reveal any issue with the stability of iPSCs. APLF, along with its interacting partner PARP3, basically promotes NHEJ (Rulten et al, 2008). Even in the absence of Aplf, overexpression of XRCC4 and DNA ligase IV leads to NHEJ repair (Rulten et al, 2008).…”

Section: Discussionmentioning

confidence: 99%

“…APLF is an important constituent of the non-homologous end joining (NHEJ)-mediated DNA damage repair machinery (Rulten et al, 2008;Grundy et al, 2013), and its downregulation in human cells could sensitize the cells to various DNA-damaging agents (Macrae et al, 2008). In order to test whether Aplf knockdown induces DNA repair defects, the cells were first challenged with actinomycin D at different concentrations and subjected to an apoptosis assay.…”

Section: Downregulation Of Aplf Enhances Reprogramming Of Fibroblastsmentioning

confidence: 99%

Histone chaperone APLF regulates induction of pluripotency in murine fibroblasts

Syed¹,

Joseph²,

Mukherjee³

et al. 2017

Development

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The authors apologise to the readers for any confusion that this error might have caused. For the first time, we report here that the downregulation of histone chaperone Aprataxin PNK-like factor (APLF) promotes reprogramming by augmenting the expression of E-cadherin (Cdh1), which is implicated in the mesenchymal-to-epithelial transition (MET) involved in the generation of induced pluripotent stem cells (iPSCs) from mouse embryonic fibroblasts (MEFs). Downregulation of APLF in MEFs expedites the loss of the repressive MacroH2A.1 (encoded by H2afy) histone variant from the Cdh1 promoter and enhances the incorporation of active histone H3me2K4 marks at the promoters of the pluripotency genes Nanog and Klf4, thereby accelerating the process of cellular reprogramming and increasing the efficiency of iPSC generation. We demonstrate a new histone chaperone (APLF)-MET-histone modification cohort that functions in the induction of pluripotency in fibroblasts. This regulatory axis might provide new mechanistic insights into perspectives of epigenetic regulation involved in cancer metastasis.

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“…PARP1 (and the closely related PARP2) is rapidly activated at sites of DNA breaks, where it catalyzes the formation of poly(ADP-ribose) (PAR) polymers both on itself (autoPARylation) and local substrates (Satoh and Lindahl, 1992;Ame et al, 1999;Allinson et al, 2003;Woodhouse and Dianov, 2008). DNA damage associated PARylation, either directly or through the recruitment of proteins such as APLF and the chromatin remodeling enzyme ALC1, induces changes in local chromatin structure that lead to chromatin relaxation and recruitment of other DNA repair proteins (Tulin and Spradling, 2003;Ahel et al, 2008;Rulten et al, 2008;Gottschalk et al, 2009).…”

Section: Brca1 and Dna Repairmentioning

confidence: 99%

BRCA1, PARP, and 53BP1: conditional synthetic lethality and synthetic viability

Aly¹,

Ganesan²

2011

Journal of Molecular Cell Biology

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BRCA1 plays a critical role in the regulation of homologous recombination (HR)-mediated DNA double-strand break repair. BRCA1-deficient cancers have evolved to tolerate loss of BRCA1 function. This renders them vulnerable to agents, such as PARP inhibitors, that are conditionally 'synthetic lethal' with their underlying repair defect. Recent studies demonstrate that BRCA1-deficient cells may acquire resistance to these agents by partially correcting their defect in HR-mediated repair, either through reversion mutations in BRCA1 or through 'synthetic viable' loss of 53BP1. These findings and their clinical implications will be reviewed in this article.

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APLF (C2orf13) Is a Novel Component of Poly(ADP-Ribose) Signaling in Mammalian Cells

Cited by 88 publications

References 35 publications

Poly(ADP-ribose) binding to Chk1 at stalled replication forks is required for S-phase checkpoint activation

Poly(ADP-ribose) binding to Chk1 at stalled replication forks is required for S-phase checkpoint activation

Histone chaperone APLF regulates induction of pluripotency in murine fibroblasts

BRCA1, PARP, and 53BP1: conditional synthetic lethality and synthetic viability

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