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Comprehensive mutational scanning of EGFR reveals TKI sensitivities of extracellular domain mutants

EGFR mutations are frequent in glioblastoma and lung cancer. Here, the authors perform deep mutational scanning of EGFR, followed by a high-throughput functional screen and analysis of patient data, to identify variants with differing sensitivities to a range of EGFR tyrosine kinase inhibitors.

Tikvah K. Hayes
Elisa Aquilanti
Matthew Meyerson
ResearchOpen Access28 Mar 2024
Nature Communications

Volume: 15, P: 1-18
Author Correction: Comprehensive mutational scanning of EGFR reveals TKI sensitivities of extracellular domain mutants

Tikvah K. Hayes
Elisa Aquilanti
Matthew Meyerson
Amendments and CorrectionsOpen Access16 Apr 2024
Nature Communications

Volume: 15, P: 1
Systematic identification of biomarker-driven drug combinations to overcome resistance

Identification of genes associated with resistance to hundreds of cancer therapeutics enabled the discovery of the serine hydrolases MGLL and CES1 as modifiers of sensitivity to GSK-J4 via direct enzymatic modification.

Matthew G. Rees
Lisa Brenan
Cory M. Johannessen
Research24 Mar 2022
Nature Chemical Biology

Volume: 18, P: 615-624
Neuronal differentiation and cell-cycle programs mediate response to BET-bromodomain inhibition in MYC-driven medulloblastoma

BET-bromodomain inhibitors could be used to treat medulloblastoma tumors with Myc amplifications. Here, the authors show that both the response and resistance to BET inhibitors in mice is mediated by bHLH/homeobox transcription factors.

Pratiti Bandopadhayay
Federica Piccioni
Rameen Beroukhim
ResearchOpen Access03 Jun 2019
Nature Communications

Volume: 10, P: 1-16

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Comprehensive mutational scanning of EGFR reveals TKI sensitivities of extracellular domain mutants

Author Correction: Comprehensive mutational scanning of EGFR reveals TKI sensitivities of extracellular domain mutants

Systematic identification of biomarker-driven drug combinations to overcome resistance

Neuronal differentiation and cell-cycle programs mediate response to BET-bromodomain inhibition in MYC-driven medulloblastoma

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