Discovery and characterization of a novel irreversible EGFR mutants selective and potent kinase inhibitor CHMFL-EGFR-26 with a distinct binding mode

EGFR T790M mutation accounts for about 40-55% drug resistance for the first generation EGFR kinase inhibitors in the NSCLC. Starting from ibrutinib, a highly potent irreversible BTK kinase inhibitor, which was also found to be moderately active to EGFR T790M mutant, we discovered a highly potent irr...

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Autores principales: Hu, Chen, Wang, Aoli, Wu, Hong, Qi, Ziping, Li, Xixiang, Yan, Xiao-E, Chen, Cheng, Yu, Kailin, Zou, Fengming, Wang, Wenchao, Wang, Wei, Wu, Jiaxin, Liu, Juan, Wang, Beilei, Wang, Li, Ren, Tao, Zhang, Shanchun, Yun, Cai-Hong, Liu, Jing, Liu, Qingsong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2017
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5392334/
https://www.ncbi.nlm.nih.gov/pubmed/28407693
http://dx.doi.org/10.18632/oncotarget.15443
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author Hu, Chen
Wang, Aoli
Wu, Hong
Qi, Ziping
Li, Xixiang
Yan, Xiao-E
Chen, Cheng
Yu, Kailin
Zou, Fengming
Wang, Wenchao
Wang, Wei
Wu, Jiaxin
Liu, Juan
Wang, Beilei
Wang, Li
Ren, Tao
Zhang, Shanchun
Yun, Cai-Hong
Liu, Jing
Liu, Qingsong
author_facet Hu, Chen
Wang, Aoli
Wu, Hong
Qi, Ziping
Li, Xixiang
Yan, Xiao-E
Chen, Cheng
Yu, Kailin
Zou, Fengming
Wang, Wenchao
Wang, Wei
Wu, Jiaxin
Liu, Juan
Wang, Beilei
Wang, Li
Ren, Tao
Zhang, Shanchun
Yun, Cai-Hong
Liu, Jing
Liu, Qingsong
author_sort Hu, Chen
collection PubMed
description EGFR T790M mutation accounts for about 40-55% drug resistance for the first generation EGFR kinase inhibitors in the NSCLC. Starting from ibrutinib, a highly potent irreversible BTK kinase inhibitor, which was also found to be moderately active to EGFR T790M mutant, we discovered a highly potent irreversible EGFR inhibitor CHMFL-EGFR-26, which is selectively potent against EGFR mutants including L858R, del19, and L858R/T790M. It displayed proper selectivity window between the EGFR mutants and the wide-type. CHMFL-EGFR-26 exhibited good selectivity profile among 468 kinases/mutants tested (S score (1)=0.02). In addition, X-ray crystallography revealed a distinct “DFG-in” and “cHelix-out” inactive binding mode between CHMFL-EGFR-26 and EGFR T790M protein. The compound showed highly potent anti-proliferative efficacy against EGFR mutant but not wide-type NSCLC cell lines through effective inhibition of the EGFR mediated signaling pathway, induction of apoptosis and arresting of cell cycle progression. CHMFL-EGFR-26 bore acceptable pharmacokinetic properties and demonstrated dose-dependent tumor growth suppression in the H1975 (EGFR L858R/T790M) and PC-9 (EGFR del19) inoculated xenograft mouse models. Currently CHMFL-EGFR-26 is undergoing extensive pre-clinical evaluation for the clinical trial purpose.
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spelling pubmed-53923342017-04-21 Discovery and characterization of a novel irreversible EGFR mutants selective and potent kinase inhibitor CHMFL-EGFR-26 with a distinct binding mode Hu, Chen Wang, Aoli Wu, Hong Qi, Ziping Li, Xixiang Yan, Xiao-E Chen, Cheng Yu, Kailin Zou, Fengming Wang, Wenchao Wang, Wei Wu, Jiaxin Liu, Juan Wang, Beilei Wang, Li Ren, Tao Zhang, Shanchun Yun, Cai-Hong Liu, Jing Liu, Qingsong Oncotarget Research Paper EGFR T790M mutation accounts for about 40-55% drug resistance for the first generation EGFR kinase inhibitors in the NSCLC. Starting from ibrutinib, a highly potent irreversible BTK kinase inhibitor, which was also found to be moderately active to EGFR T790M mutant, we discovered a highly potent irreversible EGFR inhibitor CHMFL-EGFR-26, which is selectively potent against EGFR mutants including L858R, del19, and L858R/T790M. It displayed proper selectivity window between the EGFR mutants and the wide-type. CHMFL-EGFR-26 exhibited good selectivity profile among 468 kinases/mutants tested (S score (1)=0.02). In addition, X-ray crystallography revealed a distinct “DFG-in” and “cHelix-out” inactive binding mode between CHMFL-EGFR-26 and EGFR T790M protein. The compound showed highly potent anti-proliferative efficacy against EGFR mutant but not wide-type NSCLC cell lines through effective inhibition of the EGFR mediated signaling pathway, induction of apoptosis and arresting of cell cycle progression. CHMFL-EGFR-26 bore acceptable pharmacokinetic properties and demonstrated dose-dependent tumor growth suppression in the H1975 (EGFR L858R/T790M) and PC-9 (EGFR del19) inoculated xenograft mouse models. Currently CHMFL-EGFR-26 is undergoing extensive pre-clinical evaluation for the clinical trial purpose. Impact Journals LLC 2017-02-17 /pmc/articles/PMC5392334/ /pubmed/28407693 http://dx.doi.org/10.18632/oncotarget.15443 Text en Copyright: © 2017 Hu et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Hu, Chen
Wang, Aoli
Wu, Hong
Qi, Ziping
Li, Xixiang
Yan, Xiao-E
Chen, Cheng
Yu, Kailin
Zou, Fengming
Wang, Wenchao
Wang, Wei
Wu, Jiaxin
Liu, Juan
Wang, Beilei
Wang, Li
Ren, Tao
Zhang, Shanchun
Yun, Cai-Hong
Liu, Jing
Liu, Qingsong
Discovery and characterization of a novel irreversible EGFR mutants selective and potent kinase inhibitor CHMFL-EGFR-26 with a distinct binding mode
title Discovery and characterization of a novel irreversible EGFR mutants selective and potent kinase inhibitor CHMFL-EGFR-26 with a distinct binding mode
title_full Discovery and characterization of a novel irreversible EGFR mutants selective and potent kinase inhibitor CHMFL-EGFR-26 with a distinct binding mode
title_fullStr Discovery and characterization of a novel irreversible EGFR mutants selective and potent kinase inhibitor CHMFL-EGFR-26 with a distinct binding mode
title_full_unstemmed Discovery and characterization of a novel irreversible EGFR mutants selective and potent kinase inhibitor CHMFL-EGFR-26 with a distinct binding mode
title_short Discovery and characterization of a novel irreversible EGFR mutants selective and potent kinase inhibitor CHMFL-EGFR-26 with a distinct binding mode
title_sort discovery and characterization of a novel irreversible egfr mutants selective and potent kinase inhibitor chmfl-egfr-26 with a distinct binding mode
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5392334/
https://www.ncbi.nlm.nih.gov/pubmed/28407693
http://dx.doi.org/10.18632/oncotarget.15443
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