Identifying the Appropriate FISH Criteria for Defining MET Copy Number–Driven Lung Adenocarcinoma through Oncogene Overlap Analysis

Noonan, Sinéad; Berry, Lynne D.; Lu, Xian; Gao, Dexiang; Barón, Anna E.; Chesnut, Patrick; Sheren, Jamie; Aisner, Dara L.; Merrick, Dan; Doebele, Robert C.; Varella‐Garcia, Marileila; Camidge, D. Ross

doi:10.1016/j.jtho.2016.04.033

Cited by 147 publications

(148 citation statements)

References 40 publications

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“…One drawback with FISH was the question of what cutoff should be used to predict sensitivity to MET inhibitors. A recent study by Noonan et al sheds light on the matter as it showed that a FISH MET/CEP7 ratio of ≥5 was associated with the most sensitivity to MET inhibition (49). While circulatingtumor DNA (ctDNA) testing might be a good option for capturing MET point mutations, however it is less sensitive to detect copy number changes and gene rearrangements.…”

Section: Met Inhibition For Bypass Signalingmentioning

confidence: 99%

Emerging uses of biomarkers in lung cancer management: molecular mechanisms of resistance

2017

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Management of patients with advanced non-small cell lung cancer (NSCLC) has recently been transformed by molecularly targeted and immunotherapeutic agents. In patients with EGFR/ALK/ ROS mutated NSCLC, first line molecular therapy is the standard of care. Moreover, immune checkpoint inhibitors are revolutionary treatment options for advanced NSCLC and are now the standard of care in front-line or later line settings. Both classes of agents have led to improved patient outcomes, however, primary resistance and development of acquired resistance to both targeted and immunotherapeutic agents is commonly observed, limiting the use of these agents in clinical settings. In this review, we will discuss the most recent advances in understanding the mechanisms of primary and acquired resistance, progress in the spectrum of assays detecting causative molecular events and the development of new generations of inhibitors to overcome acquired resistance.

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Section: Met Inhibition For Bypass Signalingmentioning

confidence: 99%

Emerging uses of biomarkers in lung cancer management: molecular mechanisms of resistance

2017

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“…Its role in the treatment naïve setting has also been investigated using copy number cutoffs (37). Patients with high copy number are reported to be an indicator of a more aggressive disease (38).…”

Section: Met Amplification and Met Exon 14 Skippingmentioning

confidence: 99%

“…Patients with high copy number are reported to be an indicator of a more aggressive disease (38). Complicating the interpretation of these cutoffs, is the fact that MET copy number gain, can occur in the context of focal amplification, polysomy (likely a reflection of ploidy) and even with other genomic alterations e.g., EGFR, KRAS in up to 56% of cases using a 5 copy threshold (37). Thus while MET fluorescent in situ hybridization (FISH) has been largely adopted to pre-select patients for trials, it is important to note that concurrent screening with broader next generation sequencing to exclude other drivers or immunohistochemistry (IHC) to ascertain protein expression may be complementary and allow further enrichment for potential c-MET addicted tumors (39).…”

Section: Met Amplification and Met Exon 14 Skippingmentioning

confidence: 99%

Expanded molecular interrogation for potential actionable targets in non-squamous non-small cell lung cancer

et al. 2017

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The advent of targeted therapies has established new standards of care for defined molecular subsets of non-small cell lung cancer (NSCLC). Not only has this led to significant changes in the routine clinical management of lung cancer e.g., multiplexed genomic testing, but it has provided important principles and benchmarks for determining "actionability". At present, the clinical paradigms are most evolved for EGFR mutations and ALK rearrangements, where multiple randomized phase III trials have determined optimal treatment strategies in both treatment naïve and resistant settings. However, this may not always be feasible with low prevalence alterations e.g., ROS1 and BRAF mutations. Another emerging observation is that not all targets are equally "actionable", necessitating a rigorous preclinical, clinical and translational framework to prosecute new targets and drug candidates. In this review, we will cover the role of targeted therapies for NSCLC harbouring BRAF, MET, HER2 and RET alterations, all of which have shown promise in non-squamous non-small cell lung cancer (ns-NSCLC). We further review some early epigenetic targets in NSCLC, an area of emerging interest. With increased molecular segmentation of lung cancer, we discuss the upcoming challenges in drug development and implementation of precision oncology approaches, especially in light of the complex and rapidly evolving therapeutic landscape.

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“…One approach defined the cutoff for MET gene amplification by exploiting the mutually exclusive nature of more than one driver gene aberration (17). Here we present an alternative approach of characterizing tumor cells for MET signaling-associated protein complexes.…”

Section: Introductionmentioning

confidence: 99%

MET–GRB2 Signaling-Associated Complexes Correlate with Oncogenic MET Signaling and Sensitivity to MET Kinase Inhibitors

Smith

Licata

Lakhani

et al. 2017

Clinical Cancer Research

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Purpose Targeting MET in cancer is hampered by lack of diagnostics that accurately reflect high MET signaling and dependence. We hypothesized that assays reflecting MET signaling associated protein complexes could redefine tumors dependent on MET and could add additional precision beyond genomic assessments. Experimental Design We utilized biochemical approaches, cellular viability studies and proximity ligation assays to assess MET dependence. We examined MET signaling complexes in lung cancer patient specimens (N=406) and patient-derived xenograft models of solid tumors (N=308). We evaluated response to crizotinib in a MET-amplified cohort of patient-derived xenografts models of lung cancer (N=6) and provide a case report of a lung cancer patient harboring a Δexon14 MET splice variant. Results We found the interaction of MET with the adaptor protein GRB2 is necessary for oncogenic survival signaling by MET. MET:GRB2 complexes were identified only within MET-amplified patient-derived xenograft (PDX) models and patient specimens but exhibit substantial variability. Lack of MET:GRB2 complexes was associated with lack of response to MET TKI in cell lines and PDX models. Presence of MET:GRB2 complexes can further sub type tumors with Δexon14 MET splice variants. Presence of these complexes correlated with response to crizotinib in one patient with Δexon14 MET lacking MET gene amplification. Conclusions Proximity assays measuring MET:GRB2 signaling complexes provide novel insights into MET-mediated signaling and could complement current clinical genomics-based assay platforms.

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Identifying the Appropriate FISH Criteria for Defining MET Copy Number–Driven Lung Adenocarcinoma through Oncogene Overlap Analysis

Cited by 147 publications

References 40 publications

Emerging uses of biomarkers in lung cancer management: molecular mechanisms of resistance

Emerging uses of biomarkers in lung cancer management: molecular mechanisms of resistance

Expanded molecular interrogation for potential actionable targets in non-squamous non-small cell lung cancer

MET–GRB2 Signaling-Associated Complexes Correlate with Oncogenic MET Signaling and Sensitivity to MET Kinase Inhibitors

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