Litcius/Paper detail

Discovery of Novel Macrocyclic MERTK/AXL Dual Inhibitors

Deyu Kong, Qiang Tian, Zhilong Chen, Hongchao Zheng, Michael A. Stashko, Dan Yan, H. Shelton Earp, Stephen V. Frye, Deborah DeRyckere, Dmitri Kireev, Douglas K. Graham, Xiaodong Wang

2024Journal of Medicinal Chemistry10 citationsDOIOpen Access PDF

Abstract

MERTK and AXL are members of the TAM (TYRO3, AXL, MERTK) family of receptor tyrosine kinases that are aberrantly expressed and have been implicated as therapeutic targets in a wide variety of human tumors. Dual MERTK and AXL inhibition could provide antitumor action mediated by both direct tumor cell killing and modulation of the innate immune response in some tumors such as nonsmall cell lung cancer. We utilized our knowledge of MERTK inhibitors and a structure-based drug design approach to discover a novel class of macrocyclic dual MERTK/AXL inhibitors. The lead compound 43 had low-nanomolar activity against both MERTK and AXL and good selectivity over TYRO3 and FLT3. Its target engagement and selectivity were also confirmed by NanoBRET and cell-based MERTK and AXL phosphorylation assays. Compound 43 had excellent pharmacokinetic properties (large AUC and long half-life) and mediated antitumor activity against lung cancer cell lines, indicating its potential as a therapeutic agent.

Topics & Concepts

MERTKGAS6ChemistryAXL receptor tyrosine kinaseCancer researchReceptor tyrosine kinaseCancerPharmacologyKinaseBiochemistryMedicineInternal medicineJAK-STAT signaling pathwayPhagocytosis and Immune Regulation