Adaptive Darwinian off-target resistance mechanisms to selective RET inhibition in RET driven cancer

Subbiah, Vivek; Gouda, Mohamed A.; Iorgulescu, J. Bryan; Dadu, Ramona; Patel, Keyur; Sherman, Steven; Cabanillas, Maria; Hu, Mimi; Castellanos, Luz E.; Amini, Behrang; Meric-Bernstam, Funda; Shen, Tao; Wu, Jie

doi:10.1038/s41698-024-00563-4

Cited by 6 publications

(1 citation statement)

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“…Acquired KHDRBS1-NTRK3 fusion has been reported in patients with KIF5B-RET-fusion lung cancer after selpercatinib treatment, along with RET-altered cancers exhibiting NTRK and ALK fusions. This indicates a potential dual inhibition strategy targeting TRK and ALK [115]. RET fusion, similar to MET amplification, is a mechanism of acquired resistance to osimertinib in EGFR mutation-positive NSCLC.…”

Section: Proto-oncogene Tyrosine-protein Kinase Receptor (Ret)mentioning

confidence: 95%

Kinase Inhibitors and Kinase-Targeted Cancer Therapies: Recent Advances and Future Perspectives

Li,

Gong,

Zhou

et al. 2024

IJMS

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Over 120 small-molecule kinase inhibitors (SMKIs) have been approved worldwide for treating various diseases, with nearly 70 FDA approvals specifically for cancer treatment, focusing on targets like the epidermal growth factor receptor (EGFR) family. Kinase-targeted strategies encompass monoclonal antibodies and their derivatives, such as nanobodies and peptides, along with innovative approaches like the use of kinase degraders and protein kinase interaction inhibitors, which have recently demonstrated clinical progress and potential in overcoming resistance. Nevertheless, kinase-targeted strategies encounter significant hurdles, including drug resistance, which greatly impacts the clinical benefits for cancer patients, as well as concerning toxicity when combined with immunotherapy, which restricts the full utilization of current treatment modalities. Despite these challenges, the development of kinase inhibitors remains highly promising. The extensively studied tyrosine kinase family has 70% of its targets in various stages of development, while 30% of the kinase family remains inadequately explored. Computational technologies play a vital role in accelerating the development of novel kinase inhibitors and repurposing existing drugs. Recent FDA-approved SMKIs underscore the importance of blood–brain barrier permeability for long-term patient benefits. This review provides a comprehensive summary of recent FDA-approved SMKIs based on their mechanisms of action and targets. We summarize the latest developments in potential new targets and explore emerging kinase inhibition strategies from a clinical perspective. Lastly, we outline current obstacles and future prospects in kinase inhibition.

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Section: Proto-oncogene Tyrosine-protein Kinase Receptor (Ret)mentioning

confidence: 95%