RÉSUMÉ
BACKGROUND: In preclinical gastric cancer (GC) models, FGFR2 amplification was associated with increased tumour cell proliferation and survival, and drugs targeting this pathway are now in clinical trials. METHODS: FGFR2 FISH was performed on 961 GCs from the United Kingdom, China and Korea, and the relationship with clinicopathological data and overlap with HER2 amplification were analysed. RESULTS: The prevalence of FGFR2 amplification was similar between the three cohorts (UK 7.4%, China 4.6% and Korea 4.2%), and intratumoral heterogeneity was observed in 24% of FGFR2 amplified cases. FGFR2 amplification was associated with lymph node metastases (P<0.0001). FGFR2 amplification and polysomy were associated with poor overall survival (OS) in the Korean (OS: 1.83 vs 6.17 years, P=0.0073) and UK (OS: 0.45 vs 1.9 years, P<0.0001) cohorts, and FGFR2 amplification was an independent marker of poor survival in the UK cohort (P=0.0002). Co-amplification of FGFR2 and HER2 was rare, and when high-level amplifications did co-occur these were detected in distinct areas of the tumour. CONCLUSION: A similar incidence of FGFR2 amplification was found in Asian and UK GCs and was associated with lymphatic invasion and poor prognosis. This study also shows that HER2 and FGFR2 amplifications are mostly exclusive.
Sujet(s)
Marqueurs biologiques tumoraux/génétique , Amplification de gène , Régulation de l'expression des gènes tumoraux , Récepteur ErbB-2/génétique , Récepteur FGFR2/génétique , Tumeurs de l'estomac/génétique , Tumeurs de l'estomac/mortalité , Adolescent , Adulte , Sujet âgé , Sujet âgé de 80 ans ou plus , Chine , Études de cohortes , Femelle , Humains , Hybridation fluorescente in situ , Métastase lymphatique , Mâle , Adulte d'âge moyen , Pronostic , République de Corée , Tumeurs de l'estomac/anatomopathologie , Survie , Royaume-Uni , Jeune adulteRÉSUMÉ
Fibroblast growth factor receptors (FGFRs) can act as driving oncoproteins in certain cancers, making them attractive drug targets. Here we have characterized tumour cell responses to two new inhibitors of FGFR1-3, AZ12908010 and the clinical candidate AZD4547, making comparisons with the well-characterized FGFR inhibitor PD173074. In a panel of 16 human tumour cell lines, the anti-proliferative activity of AZ12908010 or AZD4547 was strongly linked to the presence of deregulated FGFR signalling, indicating that addiction to deregulated FGFRs provides a therapeutic opportunity for selective intervention. Acquired resistance to targeted tyrosine kinase inhibitors is a growing problem in the clinic but has not yet been explored for FGFR inhibitors. To assess how FGFR-dependent tumour cells adapt to long-term FGFR inhibition, we generated a derivative of the KMS-11 myeloma cell line (FGFR(Y373C)) with acquired resistance to AZ12908010 (KMS-11R cells). Basal phosphorylated FGFR and FGFR-dependent downstream signalling were constitutively elevated and refractory to drug in KMS-11R cells. Sequencing of FGFR3 in KMS-11R cells revealed the presence of a heterozygous mutation at the gatekeeper residue, encoding FGFR3(V555M); consistent with this, KMS-11R cells were cross-resistant to AZD4547 and PD173074. These results define the selectivity and efficacy of two new FGFR inhibitors and identify a secondary gatekeeper mutation as a mechanism of acquired resistance to FGFR inhibitors that should be anticipated as clinical evaluation proceeds.
Sujet(s)
Antinéoplasiques/pharmacologie , Tumeurs/traitement médicamenteux , Récepteurs à activité tyrosine kinase/antagonistes et inhibiteurs , Récepteur de type 3 des facteurs de croissance fibroblastique/génétique , Récepteur facteur croissance fibroblaste/antagonistes et inhibiteurs , Benzamides/pharmacologie , Tumeurs du sein/traitement médicamenteux , Lignée cellulaire tumorale , Résistance aux médicaments antinéoplasiques/génétique , Femelle , Humains , Myélome multiple/traitement médicamenteux , Myélome multiple/génétique , Mutation , Pipérazines/pharmacologie , Pyrazoles/pharmacologie , Pyrimidines/pharmacologie , Récepteurs à activité tyrosine kinase/effets des médicaments et des substances chimiques , Récepteur FGFR1/antagonistes et inhibiteurs , Récepteur FGFR1/métabolisme , Récepteur FGFR2/antagonistes et inhibiteurs , Récepteur FGFR2/métabolisme , Récepteur de type 3 des facteurs de croissance fibroblastique/antagonistes et inhibiteurs , Récepteur facteur croissance fibroblaste/métabolisme , Transduction du signal/effets des médicaments et des substances chimiques , Tumeurs de l'estomac/traitement médicamenteux , Tumeurs de la vessie urinaire/traitement médicamenteuxRÉSUMÉ
Myc is overexpressed in many cancers as a result of gene rearrangement or amplification, but coding sequence changes which cluster in the N-terminal transactivation domain also appear to play a role in tumour progression. The prototypic v-Myc gene of MC29 virus differs from avian c-Myc by a series of mutations, including a change at a regulatory phosphorylation site within the mutational hotspot (thr-61) which is known to potentiate transformation in vitro. We now show that the mutation at thr-61 stabilizes the v-Myc protein (turnover difference) and that this single mutation is both necessary and sufficient for the phenotype. A major involvement of the proteasome in Myc degradation was confirmed, but surprisingly, a dilysine motif adjacent to thr-61 proved not to be the ubiquitin target. Two other v-Myc genes which carry a mutation at thr-61 (avian MH2) or a large deletion encompassing this domain (feline T17) were found to be stabilized to a similar extent as MC29, showing that stabilization is a common feature of independently derived Myc oncogenes. These results suggest a common selective process in the genesis of these three viral oncoproteins and a mechanistic link with Jun, Fos and Myb oncoproteins which are also stabilized relative to their cellular counterparts.
