The targetable kinase PIM1 drives ALK inhibitor resistance in high-risk neuroblastoma independent of MYCN status

Trigg, Ricky M; Lee, Liam C.; Prokoph, Nina; Jahangiri, Leila; Reynolds, C. Patrick; Burke, G.A. Amos; Probst, Nicola A.; Han, Miaojun; Matthews, Jamie; Lim, Hong Kai; Manners, Eleanor; Martı́nez, Sonia; Pastor, Joaquı́n; Blanco‐Aparicio, Carmen; Merkel, Olaf; Alonso, Ines Garces de los Fayos; Kodajova, Petra; Tangermann, Simone; Högler, Sandra; Luo, Ji; Kenner, Lukas; Turner, Suzanne

doi:10.1038/s41467-019-13315-x

Cited by 32 publications

(29 citation statements)

References 59 publications

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“…Other mutations included NRAS, BRCA1/2 , APC , MAP3K1 , BRAF , and CDKN2A/B copy-number variants ( Yoda et al 2018 ). Specific to neuroblastoma, bypass signaling pathways such as activation of AXL ( Debruyne et al 2016 ), PIM1 ( Trigg et al 2019 ), EGFR, and ERBB4 ( Redaelli et al 2018 ) have been reported in association with ALK TKI resistance. As the ALK F1174L mutation persisted in our patient after relapse on lorlatinib, ALK-independent mechanisms were the likely drivers of resistance.…”

Section: Discussionmentioning

confidence: 99%

Exceptional response to the ALK and ROS1 inhibitor lorlatinib and subsequent mechanism of resistance in relapsed ALK F1174L-mutated neuroblastoma

Liu

Merguerian

Rowe

et al. 2021

Cold Spring Harb Mol Case Stud

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Treatment of high-risk neuroblastoma typically incorporates multi-agent chemotherapy, surgery, radiation therapy, autologous stem cell transplantation, immunotherapy, and differentiation therapy. The discovery of activating mutations in ALK receptor tyrosine kinase (ALK) in approximately 8% of neuroblastomas opens the possibility of further improving outcomes for this subset of patients with the addition of ALK inhibitors. ALK inhibitors have shown efficacy in tumors such as non-small cell lung cancer and anaplastic large cell lymphoma where wild-type ALK overexpression is driven by translocation events. In contrast, ALK mutations driving neuroblastomas are missense mutations in the tyrosine kinase domain yielding constitutive activation and differing sensitivity to available ALK inhibitors. We describe a case of a patient with relapsed, refractory, metastatic ALK F1174L-mutated neuroblastoma who showed no response to the first generation ALK inhibitor crizotinib but had a subsequent complete response to the ALK/ROS1 inhibitor lorlatinib. The patient's disease relapsed after 13 months of treatment. Sequencing of cell-free DNA at the time of relapse pointed toward a potential mechanism of acquired lorlatinib resistance: amplification of CDK4 and FGFR1, and a NRAS Q61K mutation. We review the literature regarding differing sensitivity of ALK mutations found in neuroblastoma to current FDA-approved ALK inhibitors and known pathways of acquired resistance. Our report adds to the literature of important correlations between neuroblastoma ALK mutation status and clinical responsiveness to ALK inhibitors. It also highlights the importance of understanding acquired mechanisms of resistance.

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Section: Discussionmentioning

confidence: 99%

Exceptional response to the ALK and ROS1 inhibitor lorlatinib and subsequent mechanism of resistance in relapsed ALK F1174L-mutated neuroblastoma

Liu

Merguerian

Rowe

et al. 2021

Cold Spring Harb Mol Case Stud

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“…This analysis again highlighted our finding of MEIS2 as a putative key early dependency during murine TH-MYCN-driven neuroblastoma. In addition, other putative interesting candidates include amongst others CBX2 (a core PRC1 subunit required for binding to H3K27me3 marked domains), CDCA8 (a subunit of the “Chromosomal Passenger complex” (CPC) and direct MYCN target gene contributing to the aggressive phenotype of MYCN-amplified neuroblastoma [ 77 ]), Claspin (a key mediator of the ATR-CHK1 pathway), and PIM1 (a key driver of ALK inhibitor resistance in neuroblastoma [ 78 ]). Last, our study defined for the first time through a cross-species integrative transcriptomics approach putative master regulators for MYCN-driven neuroblastoma tumor development and revealed FOXM1 and the DREAM complex members MYBL2 and E2F8 as top-scoring candidates.…”

Section: Discussionmentioning

confidence: 99%

MEIS2 Is an Adrenergic Core Regulatory Transcription Factor Involved in Early Initiation of TH-MYCN-Driven Neuroblastoma Formation

Wyn

Zimmerman

Weichert-Leahey

et al. 2021

Cancers

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Roughly half of all high-risk neuroblastoma patients present with MYCN amplification. The molecular consequences of MYCN overexpression in this aggressive pediatric tumor have been studied for decades, but thus far, our understanding of the early initiating steps of MYCN-driven tumor formation is still enigmatic. We performed a detailed transcriptome landscaping during murine TH-MYCN-driven neuroblastoma tumor formation at different time points. The neuroblastoma dependency factor MEIS2, together with ASCL1, was identified as a candidate tumor-initiating factor and shown to be a novel core regulatory circuit member in adrenergic neuroblastomas. Of further interest, we found a KEOPS complex member (gm6890), implicated in homologous double-strand break repair and telomere maintenance, to be strongly upregulated during tumor formation, as well as the checkpoint adaptor Claspin (CLSPN) and three chromosome 17q loci CBX2, GJC1 and LIMD2. Finally, cross-species master regulator analysis identified FOXM1, together with additional hubs controlling transcriptome profiles of MYCN-driven neuroblastoma. In conclusion, time-resolved transcriptome analysis of early hyperplastic lesions and full-blown MYCN-driven neuroblastomas yielded novel components implicated in both tumor initiation and maintenance, providing putative novel drug targets for MYCN-driven neuroblastoma.

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“…PDX models of ALK mutant neuroblastoma have been pivotal in recommending particular ALK targeting small molecules for clinical studies. Of particular note, the Felix neuroblastoma PDX, which was established post-mortem from the blood of a patient who died of ALK F1245C MYCN -non-amplified high-risk neuroblastoma, has been part of several publications to highlight the potential of synergy between ALK inhibition and chemotherapy [ 76 ], the resistance to ALK inhibition mediated by Pim1 [ 77 ], and the study of novel ALK-antibody conjugates [ 78 ]. The Felix neuroblastoma PDX harbours the third most common ALK mutation found in neuroblastoma, and it exhibits de novo resistance to the first generation ALK inhibitor, crizotinib, which mirrors that seen clinically for this subgroup of patients.…”

Section: The Development and Refinement Of Patient-derived Models For Neuroblastomamentioning

confidence: 99%

“…Extensive model characterisation should be undertaken at each in vivo passage to characterise molecular concordance with the patient tumour and exclude the possibility of murine EBV-associated lymphoma [ 41 , 42 , 43 , 44 , 45 , 52 , 72 ]. At this point, the possibilities for utilisation of a successful neuroblastoma PDX model are far-reaching and include the study of clonal dynamics [ 47 , 48 , 49 , 50 ], preclinical drug testing [ 34 , 35 , 72 , 73 , 74 , 75 , 76 , 77 , 78 , 79 ], and immunological studies by using humanized mice or switching the mouse strain for further engraftment [ 80 , 81 , 82 , 83 , 84 , 85 ].…”

Section: Figurementioning

confidence: 99%

The Promise of Patient-Derived Preclinical Models to Accelerate the Implementation of Personalised Medicine for Children with Neuroblastoma

Tucker

George

Angelini

et al. 2021

JPM

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Patient-derived preclinical models are now a core component of cancer research and have the ability to drastically improve the predictive power of preclinical therapeutic studies. However, their development and maintenance can be challenging, time consuming, and expensive. For neuroblastoma, a developmental malignancy of the neural crest, it is possible to establish patient-derived models as xenografts in mice and zebrafish, and as spheroids and organoids in vitro. These varied approaches have contributed to comprehensive packages of preclinical evidence in support of new therapeutics for neuroblastoma. We discuss here the ethical and technical considerations for the creation of patient-derived models of neuroblastoma and how their use can be optimized for the study of tumour evolution and preclinical therapies. We also discuss how neuroblastoma patient-derived models might become avatars for personalised medicine for children with this devastating disease.

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The targetable kinase PIM1 drives ALK inhibitor resistance in high-risk neuroblastoma independent of MYCN status

Cited by 32 publications

References 59 publications

Exceptional response to the ALK and ROS1 inhibitor lorlatinib and subsequent mechanism of resistance in relapsed ALK F1174L-mutated neuroblastoma

Exceptional response to the ALK and ROS1 inhibitor lorlatinib and subsequent mechanism of resistance in relapsed ALK F1174L-mutated neuroblastoma

MEIS2 Is an Adrenergic Core Regulatory Transcription Factor Involved in Early Initiation of TH-MYCN-Driven Neuroblastoma Formation

The Promise of Patient-Derived Preclinical Models to Accelerate the Implementation of Personalised Medicine for Children with Neuroblastoma

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