Optimization of an Imidazo[1,2-a]pyridine Series to Afford Highly Selective Type I1/2 Dual Mer/Axl Kinase Inhibitors with In Vivo Efficacy.

William Mccoull,Scott Boyd,Martin R. Brown,Muireann Coen,Olga Collingwood,Nichola L. Davies,Ann T. Doherty,Gary Fairley,Kristin Goldberg,Elizabeth Hardaker,Guang He,Edward J. Hennessy,Philip Hopcroft,George Hodgson,Anne Jackson,Xiefeng Jiang,Ankur Karmokar,Anne-Laure Lainé,Nicola Lindsay,Yumeng Mao,Roshini Markandu,Lindsay McMurray,Neville McLean,Lorraine Mooney,Helen Musgrove,J. Willem M. Nissink,Alexander Pflug,Venkatesh Pilla Reddy,Philip B. Rawlins,Emma Rivers,Marianne Schimpl,Graham Smith,Sharon Tentarelli,Jon Travers,Robert I Troup,Josephine Walton,Cheng Wang,Stephen D. Wilkinson,Beth Williamson,Jon Winter-Holt,Dejian Yang,Yuting Zheng,Qianxiu Zhu,Paul D. Smith

Optimization of an Imidazo[1,2-a]pyridine Series to Afford Highly Selective Type I1/2 Dual Mer/Axl Kinase Inhibitors with In Vivo Efficacy.

2021

Inhibition of Mer and Axl kinases has been implicated as a potential way to improve the efficacy of current immuno-oncology therapeutics by restoring the innate immune response in the tumor microenvironment. Highly selective dual Mer/Axl kinase inhibitors are required to validate this hypothesis. Starting from hits from a DNA-encoded library screen, we optimized an imidazo[1,2-a]pyridine series using structure-based compound design to improve potency and reduce lipophilicity, resulting in a highly selective in vivo probe compound 32. We demonstrated dose-dependent in vivo efficacy and target engagement in Mer- and Axl-dependent efficacy models using two structurally differentiated and selective dual Mer/Axl inhibitors. Additionally, in vivo efficacy was observed in a preclinical MC38 immuno-oncology model in combination with anti-PD1 antibodies and ionizing radiation.

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