Overcoming Secondary Mutations of Type II Kinase Inhibitors

Xiuqi Wang; Rosa Anna DeFilippis; Wei Yan; Neil P. Shah; Hong Yu Li

doi:10.1021/acs.jmedchem.3c01629

Overcoming Secondary Mutations of Type II Kinase Inhibitors

Xiuqi Wang, Rosa Anna DeFilippis, Wei Yan, Neil P. Shah, Hong Yu Li

Research output: Contribution to journal › Review article › peer-review

3 Scopus citations

Abstract

Type II kinase inhibitors bind in the “DFG-out” kinase conformation and are generally considered to be more potent and selective than type I inhibitors, which target a DFG-in conformation. Nine type II inhibitors are currently clinically approved, with more undergoing clinical development. Resistance-conferring secondary mutations emerged with the first series of type II inhibitors, most commonly at residues within the kinase activation loop and at the “gatekeeper” position. Recently, new inhibitors have been developed to overcome such mutations; however, mutations activating other pathways (and/or other targets) have subsequently emerged on occasion. Here, we systematically summarize the secondary mutations that confer resistance to type II inhibitors, the structural basis for resistance, newer inhibitors designed to overcome resistance, as well as the challenges and opportunities for the development of new inhibitors to overcome secondary kinase domain mutations.

Original language	English (US)
Pages (from-to)	9776-9788
Number of pages	13
Journal	Journal of Medicinal Chemistry
Volume	67
Issue number	12
DOIs	https://doi.org/10.1021/acs.jmedchem.3c01629
State	Published - Jun 27 2024
Externally published	Yes

ASJC Scopus subject areas

Molecular Medicine
Drug Discovery

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10.1021/acs.jmedchem.3c01629

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abstract = "Type II kinase inhibitors bind in the “DFG-out” kinase conformation and are generally considered to be more potent and selective than type I inhibitors, which target a DFG-in conformation. Nine type II inhibitors are currently clinically approved, with more undergoing clinical development. Resistance-conferring secondary mutations emerged with the first series of type II inhibitors, most commonly at residues within the kinase activation loop and at the “gatekeeper” position. Recently, new inhibitors have been developed to overcome such mutations; however, mutations activating other pathways (and/or other targets) have subsequently emerged on occasion. Here, we systematically summarize the secondary mutations that confer resistance to type II inhibitors, the structural basis for resistance, newer inhibitors designed to overcome resistance, as well as the challenges and opportunities for the development of new inhibitors to overcome secondary kinase domain mutations.",

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AU - Wang, Xiuqi

AU - DeFilippis, Rosa Anna

AU - Yan, Wei

AU - Shah, Neil P.

AU - Li, Hong Yu

PY - 2024/6/27

Y1 - 2024/6/27

N2 - Type II kinase inhibitors bind in the “DFG-out” kinase conformation and are generally considered to be more potent and selective than type I inhibitors, which target a DFG-in conformation. Nine type II inhibitors are currently clinically approved, with more undergoing clinical development. Resistance-conferring secondary mutations emerged with the first series of type II inhibitors, most commonly at residues within the kinase activation loop and at the “gatekeeper” position. Recently, new inhibitors have been developed to overcome such mutations; however, mutations activating other pathways (and/or other targets) have subsequently emerged on occasion. Here, we systematically summarize the secondary mutations that confer resistance to type II inhibitors, the structural basis for resistance, newer inhibitors designed to overcome resistance, as well as the challenges and opportunities for the development of new inhibitors to overcome secondary kinase domain mutations.

AB - Type II kinase inhibitors bind in the “DFG-out” kinase conformation and are generally considered to be more potent and selective than type I inhibitors, which target a DFG-in conformation. Nine type II inhibitors are currently clinically approved, with more undergoing clinical development. Resistance-conferring secondary mutations emerged with the first series of type II inhibitors, most commonly at residues within the kinase activation loop and at the “gatekeeper” position. Recently, new inhibitors have been developed to overcome such mutations; however, mutations activating other pathways (and/or other targets) have subsequently emerged on occasion. Here, we systematically summarize the secondary mutations that confer resistance to type II inhibitors, the structural basis for resistance, newer inhibitors designed to overcome resistance, as well as the challenges and opportunities for the development of new inhibitors to overcome secondary kinase domain mutations.

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Overcoming Secondary Mutations of Type II Kinase Inhibitors

Abstract

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