Targeting MET: Discovery of Small Molecule Inhibitors as Non-Small Cell Lung Cancer Therapy

Wang, Chaofan; Lu, Xiaoyun

doi:10.1021/acs.jmedchem.3c00028

Cited by 15 publications

(5 citation statements)

References 190 publications

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“…Savolitinib ( 20 ) is a small molecule inhibitor of the mesenchymal epithelial transition factor (MET) oncogene and was conditionally approved in China in 2021 for treatment of patients with nonsmall cell lung cancer with MET exon 14 skipping mutations . This mutation results in increased MET stability and expression which results in prolongation of multiple downstream signaling pathways that regulate key cellular functions including proliferation, differentiation, and cell survival .…”

Section: Oncology Drugsmentioning

confidence: 99%

Synthetic Approaches to the New Drugs Approved During 2022

France,

Lindsey,

McInturff

et al. 2024

J. Med. Chem.

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In 2022, 23 new small molecule chemical entities were approved as drugs by the United States FDA, European Union EMA, Japan PMDA, and China NMPA. This review describes the synthetic approach demonstrated on largest scale for each new drug based on patent or primary literature. The synthetic routes highlight practical methods to construct molecules, sometimes on the manufacturing scale, to access the new drugs. Ten additional drugs approved in 2021 and one approved in 2020 are included that were not covered in the previous year's review. ■ SIGNFICANCEWith a brief discussion on the disease target and development background, this review focuses on synthetic routes to access new chemical entities including small molecules, antibody drug conjugates, and this year, a radioligand therapeutic. Drugs approved worldwide are included in the review.

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Section: Oncology Drugsmentioning

confidence: 99%

Synthetic Approaches to the New Drugs Approved During 2022

France,

Lindsey,

McInturff

et al. 2024

J. Med. Chem.

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“…As an example of the insights that can be learned from the inhibitor DMS screens, we examined the profile for crizotinib, one of four FDA approved inhibitors for MET and a multitarget TKI (Cui et al, 2011;Wang and Lu, 2023;Santarpia et al, 2021). To identify mutations that show gain-of-function and loss-of-function behaviors specific to inhibitors compared to DMSO, we subtracted DMSO from all fitness scores.…”

Section: Crizotinib-met Kinase Domain Resistance Profiles Exemplify T...mentioning

confidence: 99%

“…However, without extensive documentation of the behavior of resistance and sensitizing mutations in MET towards specific TKIs, there remains a barrier towards leveraging inhibitors for specific mutational responses, optimizing inhibitor pairings, and informing rational drug design. Thousands of compounds have been screened against the MET kinase domain, and while several have undergone clinical trials, currently four MET inhibitors have received FDA approval: crizotinib, cabozantinib, tepotinib, and capmatinib (Santarpia et al, 2021;Wang and Lu, 2023). Nevertheless, the emergence of resistance not only limits the efficacy of these drugs but also poses challenges for second-line therapeutic strategies, particularly in the context of rare and novel mutations.…”

Section: Introductionmentioning

confidence: 99%

Mapping kinase domain resistance mechanisms for the MET receptor tyrosine kinase via deep mutational scanning

Estevam,

Linossi,

Rao

et al. 2024

Preprint

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Mutations in the kinase and juxtamembrane domains of the MET Receptor Tyrosine Kinase are responsible for oncogenesis in various cancers and can drive resistance to MET-directed treatments. Determining the most effective inhibitor for each mutational profile is a major challenge for MET-driven cancer treatment in precision medicine. Here, we used a deep mutational scan (DMS) of ∼5,764 MET kinase domain variants to profile the growth of each mutation against a panel of 11 inhibitors that are reported to target the MET kinase domain. We identified common resistance sites across type I, type II, and type I ½ inhibitors, unveiled unique resistance and sensitizing mutations for each inhibitor, and validated non-cross-resistant sensitivities for type I and type II inhibitor pairs. We augment a protein language model with biophysical and chemical features to improve the predictive performance for inhibitor-treated datasets. Together, our study demonstrates a pooled experimental pipeline for identifying resistance mutations, provides a reference dictionary for mutations that are sensitized to specific therapies, and offers insights for future drug development.

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“…Cellular-mesenchymal epithelial transition factor (c-Met) is an effective target in cancer treatment and c-Met inhibitors have been successively launched for the treatment of solid tumors such as lung cancer and kidney cancer . c-Met inhibitors are mainly divided into three categories (types I, II, and III; see Figure ) according to their binding patterns with the c-Met kinase domain . Based on the interaction with residue G1163 near the solvent region, type I inhibitors can be further divided into type Ia (crizotinib) and Ib (capmatinib, tepotinib, and savolitinib).…”

Section: Introductionmentioning

confidence: 99%

“…Based on the interaction with residue G1163 near the solvent region, type I inhibitors can be further divided into type Ia (crizotinib) and Ib (capmatinib, tepotinib, and savolitinib). Type Ia inhibitors have hydrophobic interactions with G1163, while type Ib inhibitors bind to the kinase domain independently of this interaction, making them more selective than type Ia inhibitors. − Type II inhibitors (cabozantinib, foretinib) generally refer to multitarget kinase inhibitors, while type III inhibitors (tivantinib) refer to allosteric inhibitors …”

Section: Introductionmentioning

confidence: 99%

Discovery of Potent and Selective c-Met Degraders for Hepatocellular Carcinoma Treatment

Min,

Yang,

Wang

et al. 2024

J. Med. Chem.

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Targeting c-Met is a clinical trend for the precise treatment of HCC, but the potential issue of acquired drug resistance cannot be ignored. Targeted protein degradation technology has demonstrated promising prospects in disease treatment and overcoming drug resistance due to its special mechanism of action. In this study, we designed and synthesized two series of novel c-Met degraders and conducted a systematic biological evaluation of the optimal compound H11. H11 exhibited good c-Met degradation activity and anti-HCC activity. Importantly, H11 also demonstrated more potent inhibitory activity against Ba/F3-TPR-MET-D1228N and Ba/F3-TPR-MET-Y1230H cell lines than did tepotinib. In summary, H11 displayed potent anti-HCC activity as a degrader and may overcome resistance to type Ib inhibitors, making it a new therapeutic strategy for HCC with MET alterations.

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Targeting MET: Discovery of Small Molecule Inhibitors as Non-Small Cell Lung Cancer Therapy

Cited by 15 publications

References 190 publications

Synthetic Approaches to the New Drugs Approved During 2022

Synthetic Approaches to the New Drugs Approved During 2022

Mapping kinase domain resistance mechanisms for the MET receptor tyrosine kinase via deep mutational scanning

Discovery of Potent and Selective c-Met Degraders for Hepatocellular Carcinoma Treatment

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