Current advances of targeting HGF/c-Met pathway in gastric cancer

Anestis, Aristomenis; Zoi, Ilianna; Karamouzis, Michalis V.

doi:10.21037/atm.2018.04.42

Cited by 32 publications

(25 citation statements)

References 82 publications

(82 reference statements)

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“…[245][246][247][248] HGF is secreted mostly from mesenchymal tissues and is currently the only known ligand for MET. Its tissue and serum expression levels are related to poor prognosis of patients with different malignant tumors, such as breast, 249 esophageal, 250 and gastric cancers, 251 and especially CRC. Patients with advanced CRC have elevated serum HGF at diagnosis and decreased levels after cancer resection.…”

Section: The Hgf/c-met Pathwaymentioning

confidence: 99%

Comprehensive review of targeted therapy for colorectal cancer

Xie

Chen

Fang

2020

Sig Transduct Target Ther

920

657

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Colorectal cancer (CRC) is among the most lethal and prevalent malignancies in the world and was responsible for nearly 881,000 cancer-related deaths in 2018. Surgery and chemotherapy have long been the first choices for cancer patients. However, the prognosis of CRC has never been satisfying, especially for patients with metastatic lesions. Targeted therapy is a new optional approach that has successfully prolonged overall survival for CRC patients. Following successes with the anti-EGFR (epidermal growth factor receptor) agent cetuximab and the anti-angiogenesis agent bevacizumab, new agents blocking different critical pathways as well as immune checkpoints are emerging at an unprecedented rate. Guidelines worldwide are currently updating the recommended targeted drugs on the basis of the increasing number of high-quality clinical trials. This review provides an overview of existing CRC-targeted agents and their underlying mechanisms, as well as a discussion of their limitations and future trends.

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Section: The Hgf/c-met Pathwaymentioning

confidence: 99%

Comprehensive review of targeted therapy for colorectal cancer

Xie

Chen

Fang

2020

Sig Transduct Target Ther

920

657

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“…It can occur by protein overexpression, gene amplification, increased HGF ligand autocrine expression, enhanced paracrine ligand-mediated stimulation, inadequate c-MET degradation, ligand-independent activation and rarely gene mutation, 19 in addition to the role of environmental conditions such as inflammation and hypoxia. 24 The most common mechanism of MET pathway abnormal activation in GC is via protein overexpression with resultant excessive kinase activation. MET protein expression on immunohistochemistry (IHC) is predominantly detected in 50-65% of GC.…”

Section: -Kinase (Pi3k)/akt Extracellular Signal-regulated Kinase (Ementioning

confidence: 99%

<p><em>MET</em> Inhibitors for the Treatment of Gastric Cancer: What’s Their Potential?</p>

Darsa¹,

Sayed²,

Abdel‐Rahman³

2020

JEP

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Gastric cancer remains a disease with a dismal prognosis. Extensive efforts to find targetable disease drivers in gastric cancer were implemented to improve patient outcomes. Beyond anti-HER2 therapy, MET pathway seems to be culprit of cancer invasiveness with MET-overexpressing tumors having poorer prognosis. Tyrosine kinase inhibitors targeting the HGF/MET pathway were studied in MET-positive gastric cancer, but no substantial benefit was proven. Some patients responded in early phase trials but later developed resistance. Others failed to show any benefit at all. Etiologies of resistance may entail inappropriate patient selection with a lack of MET detection standardization, tumor alternative pathways, variable MET amplification, and genetic variation. Optimizing MET detection techniques and better understanding the MET pathway, as well as tumor bypass mechanisms, are an absolute need to devise means to overcome resistance using targeted therapy alone, or in combination with other synergistic agents to improve outcomes of patients with MET-positive GC.

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“…Therapeutically exploiting molecular biomarkers, including MET , in EGC has been plagued by multiple barriers, among the most important of which is tumoral heterogeneity. Despite, encouraging phase II studies of c‐MET antibodies (rilotumumab, onartuzumab), larger phase III EGC studies using the same screening criteria for c‐MET positivity revealed no survival benefits, regardless of c‐MET staining [46]. Larger efforts to assess for concordance between tissue (including both primary and metastatic sites) and blood (circulating tumor DNA) in order to evaluate the effect of tumor heterogeneity on response, as well as the impact of other molecular features, such as the presence of RTK co‐amplification, may aid in refining the population who are most likely to benefit from MET‐directed therapies, either alone or in combination.…”

Section: Resultsmentioning

confidence: 99%

RevisitingMET: Clinical Characteristics and Treatment Outcomes of Patients with Locally Advanced or Metastatic,MET-Amplified Esophagogastric Cancers

et al. 2020

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Background Metastatic esophagogastric cancers (EGCs) have a poor prognosis with an approximately 5% 5‐year survival. Additional treatment approaches are needed. c‐MET gene‐amplified tumors are an uncommon but potentially targetable subset of EGC. Clinical characteristics and outcomes were evaluated in patients with MET‐amplified EGC and compared with those without MET amplification to facilitate identification of these patients and possible treatment approaches. Patients and Methods Patients with locally advanced or metastatic MET‐amplified EGC at Massachusetts General Hospital (MGH) were identified using fluorescent in situ hybridization analysis, with a gene‐to‐control ratio of ≥2.2 defined as positive. Non–MET‐amplified patients identified during the same time period who had undergone tumor genotyping and treatment at MGH were evaluated as a comparison group. Results We identified 233 patients evaluated for MET amplification from 2002 to 2019. MET amplification was seen in 28 (12%) patients versus 205 (88%) patients without amplification. Most MET‐amplified tumors occurred in either the distal esophagus (n = 9; 32%) or gastroesophageal junction (n = 10; 36%). Of MET‐amplified patients, 16 (57%) had a TP53 mutation, 5(18%) had HER2 co‐amplification, 2 (7.0%) had EGFR co‐amplification, and 1 (3.5%) had FGFR2 co‐amplification. MET‐amplified tumors more frequently had poorly differentiated histology (19/28, 68.0% vs. 66/205, 32%; p = .02). Progression‐free survival to initial treatment was substantially shorter for all MET‐amplified patients (5.6 vs. 8.8 months, p = .026) and for those with metastatic disease at presentation (4.0 vs. 7.6 months, p = .01). Overall, patients with MET amplification had shorter overall survival (19.3 vs. 24.6 months, p = .049). No difference in survival was seen between low MET‐amplified tumors (≥2.2 and <25 MET copy number) compared with highly amplified tumors (≥25 MET copy number). Conclusion MET‐amplified EGC represents a distinct clinical entity characterized by rapid progression and short survival. Ideally, the identification of these patients will provide opportunities to participate in clinical trials in an attempt to improve outcomes. Implications for Practice This article describes 233 patients who received MET amplification testing and reports (a) a positivity rate of 12%, similar to the rate of HER2 positivity in this data set; (b) the clinical characteristics of poorly differentiated tumors and nodal metastases; and (c) markedly shorter progression‐free survival and overall survival in MET‐amplified tumors. Favorable outcomes are reported for patients treated with MET inhibitors. Given the lack of published data in MET‐amplified esophagogastric cancers and the urgent clinical importance of identifying patients with MET amplification for MET‐directed therapy, this large series is a valuable addition to the literature and will have an impact on future practice.

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Current advances of targeting HGF/c-Met pathway in gastric cancer

Cited by 32 publications

References 82 publications

Comprehensive review of targeted therapy for colorectal cancer

Comprehensive review of targeted therapy for colorectal cancer

<p><em>MET</em> Inhibitors for the Treatment of Gastric Cancer: What’s Their Potential?</p>

RevisitingMET: Clinical Characteristics and Treatment Outcomes of Patients with Locally Advanced or Metastatic,MET-Amplified Esophagogastric Cancers

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