| Literature DB >> 26285778 |
Bryan D Smith1, Michael D Kaufman1, Cynthia B Leary1, Benjamin A Turner1, Scott C Wise1, Yu Mi Ahn1, R John Booth1, Timothy M Caldwell1, Carol L Ensinger1, Molly M Hood1, Wei-Ping Lu1, Tristan W Patt1, William C Patt1, Thomas J Rutkoski1, Thiwanka Samarakoon1, Hanumaiah Telikepalli1, Lakshminarayana Vogeti1, Subha Vogeti1, Karen M Yates1, Lawrence Chun2, Lance J Stewart2, Michael Clare1, Daniel L Flynn3.
Abstract
Altiratinib (DCC-2701) was designed based on the rationale of engineering a single therapeutic agent able to address multiple hallmarks of cancer (1). Specifically, altiratinib inhibits not only mechanisms of tumor initiation and progression, but also drug resistance mechanisms in the tumor and microenvironment through balanced inhibition of MET, TIE2 (TEK), and VEGFR2 (KDR) kinases. This profile was achieved by optimizing binding into the switch control pocket of all three kinases, inducing type II inactive conformations. Altiratinib durably inhibits MET, both wild-type and mutated forms, in vitro and in vivo. Through its balanced inhibitory potency versus MET, TIE2, and VEGFR2, altiratinib provides an agent that inhibits three major evasive (re)vascularization and resistance pathways (HGF, ANG, and VEGF) and blocks tumor invasion and metastasis. Altiratinib exhibits properties amenable to oral administration and exhibits substantial blood-brain barrier penetration, an attribute of significance for eventual treatment of brain cancers and brain metastases. ©2015 American Association for Cancer Research.Entities:
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Year: 2015 PMID: 26285778 DOI: 10.1158/1535-7163.MCT-14-1105
Source DB: PubMed Journal: Mol Cancer Ther ISSN: 1535-7163 Impact factor: 6.261