Feedback control of PLK1 by Apolo1 ensures accurate chromosome segregation

Xu, Leilei; Ali, Mahboob; Duan, Wenxiu; Yuan, Xiao; Garba, Fatima; Mullen, McKay; Sun, Binwen; Poser, Ina; Duan, Hequan; Lu, Jie; Tian, Ruijun; Ge, Yushu; Chu, Lingluo; Pan, Weijun; Wang, Dongmei; Hyman, Anthony; Green, Hadiyah; Li, Lin; Dou, Zhen; Liu, Dan; Liu, Xing; Yao, Xuebiao

doi:10.1016/j.celrep.2021.109343

Cited by 19 publications

(14 citation statements)

References 51 publications

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“…Alike other scaffolding proteins such as REV7, it is possible that C1orf112 forms different molecular complexes, depending on the cellular context, thereby preserving genomic stability (reviewed in 45 ). In fact, our proteomic analysis also identified ERCC6L as one of the top constitutive interactors of C1orf112, which may likely reflect a role during mitotic progression 18 .…”

Section: Discussionmentioning

confidence: 67%

“…According to this network, we found that C1orf112 behaves similarly to factors of the cellular response to ICL agent in BL cell lines. Previous reports identified C1orf112 (aka Apolo1) as a modulator of chromosome segregation through the regulation of PLK1 activity 18 . As no other genes associated with mitosis progression were enriched in our screens, we reasoned that a different function of C1orf112 may be important for the cellular response to ICL.…”

Section: Resultsmentioning

confidence: 99%

“…Two of these interactors, the Pericentriolar material 1 protein (PCM1) and the DNA excision repair protein ERCC6-like (ERCC6L, also known as PICHs), play a role in mitosis where they respectively contribute to the proper assembly of functional centrosomes and the resolution of anaphase bridges 30,31,33 . Therefore, we reasoned that they most likely play a role in the mitotic function of C1orf112 (APOLO1) (Xu et al, 2021). Interestingly, the AAA+ ATPase Fidgetin Like 1 (FIGNL1) was also identified as a constitutive interactor of C1orf112 in our mTurboID.…”

Section: C1orf112 Interacts and Acts With Fignl1 In Icl Repairmentioning

confidence: 94%

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C1orf112 is a novel regulator of interstrand crosslink that decreases FIGNL1-RAD51 interaction

Carpio¹,

Dessapt

Villot

et al. 2022

Preprint

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Interstrand DNA crosslinks (ICLs) represent complex lesions that block essential biological processes, including DNA replication, recombination, and transcription. Several pathways have been involved in ICL repair, in particular nucleotide excision repair (NER), translesion DNA synthesis (TLS), Fanconi anemia (FA), and homologous recombination (HR). Still, the extent of factors involved in the resolution of ICL-induced DNA double-strand breaks (DSBs) remains poorly defined. Using CRISPR-based genome-wide screening, we identified the poorly characterized C1orf112 (also known as Apolo1) as a novel sensitizer to the clinically relevant ICL-inducing agent mafosfamide. Consistently, we noted that low expression of C1orf112 correlates with increased sensitivity to a series of ICL agents and PARP inhibitors in a panel of cell lines. We showed that lack of C1orf112 does not impact the initial recruitment and ubiquitylation of FANCD2 at the ICL site but rather impairs the resolution of RAD51 from ICL-induced DSBs, thereby compromising homology-directed DNA repair pathways. Our proximal mapping of C1orf112 protein neighbours coupled to structure-function analysis revealed that C1orf112, through its WCF motif, forms a complex with the N-terminal domain of the AAA+ ATPase FIGNL1 and regulates the interaction of FIGNL1 with RAD51. Our work establishes the C1orf112-FIGNL1 complex as an integral part of the HR-mediated response to ICLs by regulating the unloading of RAD51 during ICL repair.

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Section: Discussionmentioning

confidence: 67%

Section: Resultsmentioning

confidence: 99%

Section: C1orf112 Interacts and Acts With Fignl1 In Icl Repairmentioning

confidence: 94%

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C1orf112 is a novel regulator of interstrand crosslink that decreases FIGNL1-RAD51 interaction

Carpio¹,

Dessapt

Villot

et al. 2022

Preprint

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“…This suggests that regulation of RAD51 dynamics alone may not fully account for the observed synthetic lethality between C1orf112 and ERCC6L , and we cannot rule out that C1orf112 has functions beyond FIGNL1 stabilisation and RAD51 filament formation. Indeed, an additional role for C1orf112 in regulating PLK1 activity during early mitosis has been described recently (Xu et al, 2021). In fact, we identified PLK1 as a potential interactor of C1orf112 in our mitotic mass spectrometry data set (Suppl.…”

Section: Discussionmentioning

confidence: 97%

The FIGNL1-interacting protein C1orf112 is synthetic lethal with PICH and mediates RAD51 retention on chromatin

Stok

Tempel

Everts

et al. 2022

Preprint

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Joint DNA molecules are natural by-products of DNA replication and repair. Persistent joint molecules give rise to ultrafine DNA bridges (UFBs) in mitosis, which compromise sister chromatid separation. The DNA translocase PICH (ERCC6L) plays a central role in UFB resolution. A genome-wide loss-of-function screen was performed to identify the genetic contexts in which cells become dependent on PICH. In addition to genes involved in DNA condensation, centromere stability and DNA damage repair, we identified the uncharacterized protein C1orf112. We find that C1orf112 interacts with and stabilizes the AAA+ ATPase FIGNL1. Inactivation of either C1orf112 or FIGNL1 resulted in UFB formation, prolonged retention of RAD51 on chromatin, impaired replication fork dynamics, and consequently impaired genome maintenance. Combined, our data reveal that inactivation of C1orf112 and FIGNL1 dysregulates RAD51 dynamics at replication forks, resulting in DNA replication defects, and a dependency on PICH to preserve cell viability.

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“…To execute its multiple roles, Cdk1 must phosphorylate its numerous substrates in a spatiotemporally controlled manner. Kinases adopt different mechanisms, such as the structure of the kinase catalytic cleft, the kinase docking site, localization of the kinase, and system‐level competition between substrates, to phosphorylate their substrates selectively (Ubersax & Ferrell, 2007; Xu et al , 2021). Cyclin B determines Cdk1 substrate selectivity through the docking domain and subcellular localization of Cdk1.…”

Section: Discussionmentioning

confidence: 99%

Mad2 promotes Cyclin B2 recruitment to the kinetochore for guiding accurate mitotic checkpoint

et al. 2022

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Accurate mitotic progression relies on the dynamic phosphorylation of multiple substrates by key mitotic kinases. Cyclin‐dependent kinase 1 is a master kinase that coordinates mitotic progression and requires its regulatory subunit Cyclin B to ensure full kinase activity and substrate specificity. The function of Cyclin B2, which is a closely related family member of Cyclin B1, remains largely elusive. Here, we show that Mad2 promotes the kinetochore localization of Cyclin B2 and that their interaction at the kinetochores guides accurate chromosome segregation. Our biochemical analyses have characterized the Mad2‐Cyclin B2 interaction and delineated a novel Mad2‐interacting motif (MIM) on Cyclin B2. The functional importance of the Cyclin B2‐Mad2 interaction was demonstrated by real‐time imaging in which MIM‐deficient mutant Cyclin B2 failed to rescue the chromosomal segregation defects. Taken together, we have delineated a previously undefined function of Cyclin B2 at the kinetochore and have established, in human cells, a mechanism of action by which Mad2 contributes to the spindle checkpoint.

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Feedback control of PLK1 by Apolo1 ensures accurate chromosome segregation

Cited by 19 publications

References 51 publications

C1orf112 is a novel regulator of interstrand crosslink that decreases FIGNL1-RAD51 interaction

C1orf112 is a novel regulator of interstrand crosslink that decreases FIGNL1-RAD51 interaction

The FIGNL1-interacting protein C1orf112 is synthetic lethal with PICH and mediates RAD51 retention on chromatin

Mad2 promotes Cyclin B2 recruitment to the kinetochore for guiding accurate mitotic checkpoint

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