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http://hdl.handle.net/10400.18/6701| Título: | Genetic alterations of ALK in high-risk neuroblastoma patients. A SIOPEN study |
| Autor: | Bellini, Angela Bernard, Virginie Ambros, Inge F. Ambros, Peter de Preter, Katleen Combaret, Valérie Beiske, Klaus Jeison, Marta Marques, Barbara Morini, Martina Mazzocco, Katia Defferrari, Raffaella Betts, David Martinsson, Tommy Mühlethaler-Mottet, Annick Noguera, Rosa Font de Mora, Jaime Vicha, Ales Ladenstein, Ruth Valteau-Couanet, Dominique Rossing, Caroline Maria Bown, Nick Tweddle, Deborah Avigad, Smadar Lapouble, Eve Chicard, Mathieu Leprovost, Nada Clement, Nathalie Baulande, Sylvain Pierron, Gaelle Irene, Jimenez Jaydutt, Bhalshankar Delattre, Olivier Michon, Jean Schleiermacher, Gudrun |
| Palavras-chave: | Neuroblastoma ALK SIOPEN Doenças Genéticas Neuroblastoma |
| Data: | 26-Out-2019 |
| Resumo: | Background: In neuroblastoma (NB), the ALK receptor tyrosine kinase can be constitutively activated through genomic amplification or activating point mutations. We studied ALK genetic alterations in high-risk NB patients to determine their frequency and prognostic impact. Methods: Diagnostic NB samples from 1039 patients enrolled in the SIOPEN-HR-NBL1 trial were studied to determine the ALK amplification status (copy number analysis; n=337), the ALK mutational profile (Sanger and/or NGS including deep sequencing, n=203) or both (n=499). The sensitivity of ALK mutated/ALK amplified or ALK wildtype NB cell lines ((CLB-GA (R1275Q), CLB-GE (F1174V; ALK-A), SKNBE-2C (ALK wt)) to simultaneous or consecutive combinations of ALK TKIs (crizotinib/lorlatinib) and/or chemotherapy (Etoposide and Doxorubicin) was then tested. Results: Genomic ALK amplifications were detected in 4.4% of cases (37/836); all but 2 showed MYCN amplification. ALK mutations were detected at a clonal level (>20% mutated allele fraction, MAF) in 9.8% of cases (69/702) (F1174 n=25, R1275 n=32, both F1174 and R1275 n=1, F1245 n=6, others n=5) and at a subclonal level (MAF 0.5-20%) in 3.7% of patients (22/586) (F1174 n=11, R1275 n=6, both F1174 and R1275 or F1174 and F1245 n=3, other n=2). A significantly poorer OS and EFS was observed in cases with clonal ALK mutations, versus all others (3-years OS 47% +/-6.4% versus 65% +/-2%, logrank, p< 0.0001) and in those with ALK amplifications, versus all others (3-years OS 31% +/-8.5% versus 66% +/- 1.9%; logrank, p<0.0001). A Cox proportional hazards procedure (450 patients with complete clinical/biological datasets) retained stage 4 disease (as opposed to non-stage 4) and ALK amplification as factors with a higher hazard of relapse/progression (hazard 2.3 and 2.2, respectively), whereas ALK mutation, MYCN amplification and age>18 months were not retained. The consecutive treatment of Doxorubicin followed by Lorlatinib had a synergistic effect in ALK mutated/amplified NB cell lines. Conclusion: Genetic alterations of ALK (clonal mutations, amplifications) in high-risk NB patients are associated with poorer survival. Further preclinical data are required to determine optimal treatment modalities for integration of TKI in upfront treatment strategies of HR NB patients with ALK alterations. |
| Peer review: | yes |
| URI: | http://hdl.handle.net/10400.18/6701 |
| Aparece nas colecções: | DGH - Posters/abstracts em congressos internacionais |
Ficheiros deste registo:
| Ficheiro | Descrição | Tamanho | Formato | |
|---|---|---|---|---|
| Abstract ALK SIOPEN SIOP2019_gs.pdf | 267,22 kB | Adobe PDF | Ver/Abrir |
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