Systematic analysis and molecular profiling of EGFR allosteric inhibitor cross-reactivity across the proto-oncogenic ErbB family kinases by integrating dynamics simulation, energetics calculation and biochemical assay

Yanli Ma; Bingli Qi; Meiying Ning; Lijuan Zhang; Zeyu An; Jing Zhao

doi:10.1007/s00249-022-01594-0

Systematic analysis and molecular profiling of EGFR allosteric inhibitor cross-reactivity across the proto-oncogenic ErbB family kinases by integrating dynamics simulation, energetics calculation and biochemical assay

Eur Biophys J. 2022 Apr;51(3):283-295. doi: 10.1007/s00249-022-01594-0. Epub 2022 Mar 21.

Authors

Yanli Ma¹, Bingli Qi², Meiying Ning¹, Lijuan Zhang¹, Zeyu An¹, Jing Zhao³

Affiliations

¹ Department of Pharmacy, Cangzhou Central Hospital, Hebei Medical University, Cangzhou, 061000, China.
² Department of Gynaecology, Cangzhou Central Hospital, Hebei Medical University, Cangzhou, 061000, China.
³ Department of Pharmacy, Cangzhou Central Hospital, Hebei Medical University, Cangzhou, 061000, China. jingzzhao@tom.com.

PMID: 35307752
DOI: 10.1007/s00249-022-01594-0

Abstract

Human ErbB family of proteins contains four receptor tyrosine kinases (EGFR, Her2, Her3 and Her4) and has been established as a group of attractive druggable targets against diverse cancers. Over the past decades, a variety of ATP-competitive inhibitors have been discovered to target the orthosteric site of EGFR, which, however, would eventually develop acquired drug resistance due to the missense mutations T790M/C797S occurring in orthosteric site. In recent years, a number of forth-generation inhibitors have been successfully designed to overcome the T790M/C797S-induced drug resistance by targeting EGFR allosteric site instead of orthosteric site. Considering that the four proto-oncogenic ErbB kinases share a high conservation in sequence, structure and function, we herein attempted to investigate the binding potency and cross-reactivity of cognate EGFR allosteric inhibitors over noncognate Her2, Her3 and Her4 kinases--they are closely related to gynecological tumors such as ovarian cancer but no allosteric inhibitors have been reported specifically for them to date. A systematic affinity profile of 12 allosteric inhibitors and 4 orthosteric inhibitors to the 4 ErbB kinases was created by integrating dynamics simulations, energetics calculations and biochemical assays, which was then used to derive a systematic inhibitor selectivity profile for EGFR over other three kinases. It is found that allosteric and orthosteric inhibitors exhibit moderate and modest cross-reactivity across the ErbB family, respectively, but the former generally has a higher binding potency than the latter due to the additional energy cost used for inducing kinase conformational change. Moreover, most allosteric inhibitors can be sensitized by Her2 T798M gatekeeper mutation, a counterpart of EGFR T790M gatekeeper mutation that has been previously reported to cause generic drug resistance for orthosteric inhibitors.

Keywords: Allosteric inhibitor; Cross-reactivity; ErbB kinase; Gatekeeper mutation; Molecular modeling; Orthosteric inhibitor; Ovarian cancer.

MeSH terms

Drug Resistance, Neoplasm
ErbB Receptors / genetics
Humans
Lung Neoplasms*
Molecular Dynamics Simulation
Mutation
Protein Kinase Inhibitors* / pharmacology

Substances

Protein Kinase Inhibitors
EGFR protein, human
ErbB Receptors