CEP131 Abrogates CHK1 Inhibitor-Induced Replication Defects and Is Associated with Unfavorable Outcome in Neuroblastoma

Ando, Kiyohiro; Cázares-Ordoñez, Verna; Makishima, Makoto; Yokoyama, Atsushi; Suenaga, Yusuke; Nagase, Hiroki; Kobayashi, Shinichi; Koshinaga, Tsugumichi; Wada, Satoshi

doi:10.1155/2020/2752417

Cited by 4 publications

(3 citation statements)

References 35 publications

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“…We demonstrate for the first time that bi-allelic loss of BARD1 confers a targetable vulnerability in this disease. In our cohort of 59 NBLs, we found 3 cases with P/LP germline mutations in HRR genes ( Figure 1 D ), consistent with recent genomic profiling of HR-NBL germline and tumor samples, which showed multiple defective DNA repair mechanisms ( ATRX , 11q LOH, ATM , H2AFX , CHK1 , CEP131 and MRE11 ) 41 – 45 . Published studies of drug exposure experiments using in vitro cell line models and in vivo zebrafish models also suggest that patients with such defects may benefit from a similar therapeutic strategy 46 – 56 .…”

supporting

confidence: 89%

Clinical Response to a PARP Inhibitor and Chemotherapy in a Child with BARD1-Mutated Refractory Neuroblastoma: A Case Report

Federico,

Cupit-Link,

Hagiwara

et al. 2023

Preprint

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Despite advances in the treatment of high-risk neuroblastoma, approximately half of these patients die from the disease. Targeted therapy based on synthetic lethality associated with homologous recombination deficiency (HRD) caused by germline mutations in homologous recombination repair genes has shown great efficacy in several adult solid tumors. Here we report the first successful treatment of a pediatric patient with refractory neuroblastoma and a germline pathogenic mutation in BARD1 using a PARP inhibitor, talazoparib, in combination with cytotoxic chemotherapy and radiation therapy. Allele-specific expression in RNA-seq indicates bi-allelic loss of BARD1 in tumor; however, the HRD score was below the threshold currently used for HRD classification in adult cancers. Our study demonstrates that the use of PARP inhibition in combination with DNA-damaging agents should be considered in children with BARD1-mutated neuroblastoma and cautions against the use of HRD score alone as a biomarker for this pediatric population.

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confidence: 89%

Clinical Response to a PARP Inhibitor and Chemotherapy in a Child with BARD1-Mutated Refractory Neuroblastoma: A Case Report

Federico,

Cupit-Link,

Hagiwara

et al. 2023

Preprint

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“…Generation of a stable cell line transduced with a lentiviral-mediated expression system was performed using the ViraPower Lentiviral Gateway Expression Kit (Invitrogen), as described previously. 26…”

Section: Construction Of Expression Vectors and Stable Cell Linesmentioning

confidence: 99%

FGFR2 loss sensitizes MYCN‐amplified neuroblastoma CHP134 cells to CHK1 inhibitor–induced apoptosis

et al. 2021

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“…Our group and others have identified Mdm2 as the main E3 ligase implicated in GRK2 turnover upon GPCR stimulation [ 33 , 34 , 35 ], although the E3 ligase targeting GRK2 during the G2 remains to be identified [ 31 ]. Interestingly, downregulation of the centrosome-associated protein CEP131 by Mdm2 has been associated with centrosome amplification [ 36 , 37 ]; however, no effects in centrosome separation have been described so far. Our results show that control of GRK2 stability by Mdm2 is an intrinsic event in the regulation of centrosome separation that counterbalances EGF-induced and GRK2-mediated activation of the MST2–Nek2A module.…”

Section: Introductionmentioning

confidence: 99%

Mdm2-Mediated Downmodulation of GRK2 Restricts Centrosome Separation for Proper Chromosome Congression

Reglero

Castillo

Rivas

et al. 2021

Cells

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The timing of centrosome separation and the distance moved apart influence the formation of the bipolar spindle, affecting chromosome stability. Epidermal growth factor receptor (EGFR) signaling induces early centrosome separation through downstream G protein-coupled receptor kinase GRK2, which phosphorylates the Hippo pathway component MST2 (Mammalian STE20-like protein kinase 2), in turn allowing NIMA kinase Nek2A activation for centrosomal linker disassembly. However, the mechanisms that counterbalance centrosome disjunction and separation remain poorly understood. We unveil that timely degradation of GRK2 by the E3 ligase Mdm2 limits centrosome separation in the G2. Both knockout expression and catalytic inhibition of Mdm2 result in GRK2 accumulation and enhanced centrosome separation before mitosis onset. Phosphorylation of GRK2 on residue S670 enables a complex pattern of non-K48-linked polyubiquitin chains assembled by Mdm2, which correlate with kinase protein degradation. Remarkably, GRK2-S670A protein fails to phosphorylate MST2 despite overcoming Mdm2-dependent degradation, which results in defective centrosome separation, shorter spindles, and abnormal chromosome congression. Conversely, extra levels of wild-type kinase in the G2 cause increased inter-centrosome distances with longer spindles, also converging in congression issues. Our findings show that the signals enabling activity of the GRK2/MST2/Nek2A axis for separation also switches on Mdm2 degradation of GRK2 to ensure accurate centrosome dynamics and proper mitotic spindle functionality.

show abstract

CEP131 Abrogates CHK1 Inhibitor-Induced Replication Defects and Is Associated with Unfavorable Outcome in Neuroblastoma

Cited by 4 publications

References 35 publications

Clinical Response to a PARP Inhibitor and Chemotherapy in a Child with BARD1-Mutated Refractory Neuroblastoma: A Case Report

Clinical Response to a PARP Inhibitor and Chemotherapy in a Child with BARD1-Mutated Refractory Neuroblastoma: A Case Report

FGFR2 loss sensitizes MYCN‐amplified neuroblastoma CHP134 cells to CHK1 inhibitor–induced apoptosis

Mdm2-Mediated Downmodulation of GRK2 Restricts Centrosome Separation for Proper Chromosome Congression

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