Characterization of Rearrangements Involving the <i>ALK</i> Gene Reveals a Novel Truncated Form Associated with Tumor Aggressiveness in Neuroblastoma

Cazes, Alex; Louis‐Brennetot, Caroline; Mazot, Pierre; Dingli, Florent; Lombard, Bérangère; Boeva, Valentina; Daveau, Romain; Cappo, Julie; Combaret, Valérie; Schleiermacher, Gudrun; Jouannet, Stéphanie; Ferrand, Sandrine; Pierron, Gaëlle; Barillot, Emmanuel; Loew, Damarys; Vigny, Marc; Delattre, Olivier; Janoueix‐Lerosey, Isabelle

doi:10.1158/0008-5472.can-12-1242

Cited by 55 publications

(61 citation statements)

References 30 publications

(55 reference statements)

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“…In order to investigate the therapeutic efficacy of brigatinib in a neuroblastoma setting we employed several neuroblastoma cell lines, including CLB-BAR (MYCN amplification, ALK (Δ4-11) and amplified, ALK addicted), CLB-GE (MYCN amplification, ALK (F1174V) amplification, ALK addicted), IMR32 (MYCN amplification, WT ALK) and CLB-PE (MYCN amplified, WT ALK) [21,[31][32][33]. We have earlier shown that both CLB-BAR and CLB-GE cell lines are ALK addicted, while IMR32 and CLB-PE are not [34,35].…”

Section: Brigatinib Inhibits Alk Activity and Abrogates Proliferationmentioning

confidence: 99%

Brigatinib, an anaplastic lymphoma kinase inhibitor, abrogates activity and growth in ALK positive neuroblastoma cells, Drosophila and mice

Siaw¹

2016

European Journal of Cancer

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Section: Brigatinib Inhibits Alk Activity and Abrogates Proliferationmentioning

confidence: 99%

Brigatinib, an anaplastic lymphoma kinase inhibitor, abrogates activity and growth in ALK positive neuroblastoma cells, Drosophila and mice

Siaw¹

2016

European Journal of Cancer

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“…The most frequent substitutions, observed in approximately 85% of mutant ALK in neuroblastoma, are localized within the kinase domain of ALK at the F1174 (mutated to L, S, I, C, or V) and R1275 (mutated to Q or L) hotspots (12,21). In neuroblastoma, ALK can also be activated by genomic amplification (approximately 1%-2% of neuroblastomas) or more rarely following structural rearrangements (22).…”

Section: Introductionmentioning

confidence: 99%

Deep Sequencing Reveals Occurrence of Subclonal ALK Mutations in Neuroblastoma at Diagnosis

Bellini

Bernard

Leroy

et al. 2015

Clinical Cancer Research

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Purpose: In neuroblastoma, activating ALK receptor tyrosine kinase point mutations play a major role in oncogenesis. We explored the potential occurrence of ALK mutations at a subclonal level using targeted deep sequencing.Experimental Design: In a clinically representative series of 276 diagnostic neuroblastoma samples, exons 23 and 25 of the ALK gene, containing the F1174 and R1275 mutation hotspots, respectively, were resequenced with an extremely high depth of coverage.Results: At the F1174 hotspot (exon 23), mutations were observed in 15 of 277 samples (range of fraction of mutated allele per sample: 0.562%-40.409%). At the R1275 hotspot (exon 25), ALK mutations were detected in 12 of 276 samples (range of fraction of mutated allele: 0.811%-73.001%). Altogether, subclonal events with a mutated allele fraction below 20% were observed in 15/27 ALK-mutated samples. The presence of an ALK mutation was associated with poorer 5-year overall survival (OS: 75% vs. 57%, P ¼ 0.0212 log-rank test), with a strong correlation between F1174 ALK mutations and MYCN amplification being observed.Conclusions: In this series, deep sequencing allows the detection of F1174 and R1275 ALK mutational events at diagnosis in 10% of cases, with subclonal events in more than half of these, which would have gone undetected by Sanger sequencing. These findings are of clinical importance given the potential role of ALK mutations in clonal evolution and relapse. These findings also demonstrate the importance of deep sequencing techniques for the identification of patients especially when considering targeted therapy.

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“…In this tumor type, characterized by mutations within the tyrosine kinase of ALK in a subset of samples, truncated ALK proteins with complete skipping of exon 2-3 ( ALK del2-3) and exons 4-11 ( ALK del4-11) of ALK have been described and characterized 24,25 . Different than the EML4-ALK del27-derived protein EML4-ALK T1312fs*0 described herein by us, these truncated extracellular domain proteins led to increased constitutive kinase activity of ALK and transformation potential (i.e., ALK del2-3 and ALK del4-11 were putative driver events).…”

Section: Resultsmentioning

confidence: 99%

Identification and Characterization of ALK Kinase Splicing Isoforms in Non–Small-Cell Lung Cancer

Figueiredo-Pontes

Wong

Tin

et al. 2014

Journal of Thoracic Oncology

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Purpose: Anaplastic lymphoma kinase (ALK) rearrangements are present in an important subset of non-small-cell lung cancer (NSCLC) and predict for response to the tyrosine kinase inhibitor crizotinib. In this study, we evaluated the yet unknown frequency and functional role of ALK splicing isoforms in NSCLC. Experimental Design: We analyzed 270 cases of NSCLC for ALK kinase domain splicing aberrations, and in addition generated constructs with full length EML4-ALK (E13;A20) and a splicing isoform. Results: Splicing isoforms of the kinase domain of ALK - including complete skipping of exon 23 (ALKdel23, ALK p.I1171fs*42) and exon 27 (ALKdel27, ALK p.T1312fs*0) - were identified in 11.1% (30/270 cases) of NSCLC, and these changes co-existed with ALK rearrangements, KRAS mutations and EGFR mutations. ALK splicing isoforms were observed with full length EML4-ALK in crizotinib-naïve and treated NSCLCs. ALK T1312fs*0 was unable to render cells solely dependent on ALK signaling. Unlike EML4-ALK and EML4-ALK p.L1196M, EML4-ALK T1312fs*0 did not autophosphorylate ALK or other phospho-tyrosine sites. Co-expression of equal amounts of EML4-ALK T1312fs*0 and EML4-ALK did not result in resistance to crizotinib, while co-expression of EML4-ALK L1196M with EML4-ALK resulted in resistance to inhibition of ALK by crizotinib. Conclusions: ALK kinase splicing isoforms were present in NSCLC and even if translated seemed to be non-functional variants of ALK.

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Characterization of Rearrangements Involving the ALK Gene Reveals a Novel Truncated Form Associated with Tumor Aggressiveness in Neuroblastoma

Cited by 55 publications

References 30 publications

Brigatinib, an anaplastic lymphoma kinase inhibitor, abrogates activity and growth in ALK positive neuroblastoma cells, Drosophila and mice

Brigatinib, an anaplastic lymphoma kinase inhibitor, abrogates activity and growth in ALK positive neuroblastoma cells, Drosophila and mice

Deep Sequencing Reveals Occurrence of Subclonal ALK Mutations in Neuroblastoma at Diagnosis

Identification and Characterization of ALK Kinase Splicing Isoforms in Non–Small-Cell Lung Cancer

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