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  • Superior Efficacy and Selectivity of Novel Small-Molecule Kinase Inhibitors of T790M-Mutant EGFR in Preclinical Models of Lung Cancer.

Superior Efficacy and Selectivity of Novel Small-Molecule Kinase Inhibitors of T790M-Mutant EGFR in Preclinical Models of Lung Cancer.

Cancer research (2017-01-14)
Jin Kyung Rho, In Yong Lee, Yun Jung Choi, Chang-Min Choi, Jae-Young Hur, Jong Sung Koh, Jaekyoo Lee, Byung-Chul Suh, Ho-Juhn Song, Paresh Salgaonkar, Jungmi Lee, Jaesang Lee, Dong Sik Jung, Sang-Yeob Kim, Dong-Cheol Woo, In-Jeoung Baek, Joo-Yong Lee, Chang Hoon Ha, Young Hoon Sung, Jeong Kon Kim, Woo Sung Kim, Joon Seon Song, Cheol Hyeon Kim, Trever G Bivona, Jae Cheol Lee
RÉSUMÉ

The clinical utility of approved EGFR small-molecule kinase inhibitors is plagued both by toxicity against wild-type EGFR and by metastatic progression in the central nervous system, a disease sanctuary site. Here, we report the discovery and preclinical efficacy of GNS-1486 and GNS-1481, two novel small-molecule EGFR kinase inhibitors that are selective for T790M-mutant isoforms of EGFR. Both agents were effective in multiple mouse xenograft models of human lung adenocarcinoma (T790M-positive or -negative), exhibiting less activity against wild-type EGFR than existing approved EGFR kinase inhibitors (including osimertinib). In addition, GNS-1486 showed superior potency against intracranial metastasis of EGFR-mutant lung adenocarcinoma. Our results offer a preclinical proof of concept for new EGFR kinase inhibitors with the potential to improve therapeutic index and efficacy against brain metastases in patients.

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WZ4002, ≥98% (HPLC)