A tyrosine kinase inhibitor-induced interferon response positively associates with clinical response in EGFR-mutant lung cancer

A tyrosine kinase inhibitor-induced interferon response positively associates with clinical response in EGFR-mutant lung cancer

Abstract Tyrosine kinase inhibitors (TKIs) targeting EGFR-mutant lung cancers promote a range of tumor regression responses to yield variable residual disease, a likely incubator for acquired resistance. Herein, rapid transcriptional responses induced by TKIs early in treatment that associate with t...

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Main Authors: Natalia J. Gurule, Caroline E. McCoach, Trista K. Hinz, Daniel T. Merrick, Adriaan Van Bokhoven, Jihye Kim, Tejas Patil, Jacob Calhoun, Raphael A. Nemenoff, Aik Choon Tan, Robert C. Doebele, Lynn E. Heasley
Format: Article
Language:English
Published: Nature Publishing Group 2021-05-01
Series:npj Precision Oncology
Online Access:https://doi.org/10.1038/s41698-021-00181-4
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spelling doaj-d5ae4b79688c4b8094ee97ddf345427d2021-05-23T11:09:55ZengNature Publishing Groupnpj Precision Oncology2397-768X2021-05-015111110.1038/s41698-021-00181-4A tyrosine kinase inhibitor-induced interferon response positively associates with clinical response in EGFR-mutant lung cancerNatalia J. Gurule0Caroline E. McCoach1Trista K. Hinz2Daniel T. Merrick3Adriaan Van Bokhoven4Jihye Kim5Tejas Patil6Jacob Calhoun7Raphael A. Nemenoff8Aik Choon Tan9Robert C. Doebele10Lynn E. Heasley11Department of Craniofacial Biology, University of Colorado Anschutz Medical CampusDepartment of Medicine and Helen Diller Family Comprehensive Cancer Center, University of CaliforniaDepartment of Craniofacial Biology, University of Colorado Anschutz Medical CampusDepartment of Pathology, University of Colorado Anschutz Medical CampusDepartment of Pathology, University of Colorado Anschutz Medical CampusDepartment of Medicine, University of Colorado Anschutz Medical CampusDepartment of Medicine, University of Colorado Anschutz Medical CampusDepartment of Craniofacial Biology, University of Colorado Anschutz Medical CampusDepartment of Medicine, University of Colorado Anschutz Medical CampusMoffitt Cancer CenterDepartment of Medicine, University of Colorado Anschutz Medical CampusDepartment of Craniofacial Biology, University of Colorado Anschutz Medical CampusAbstract Tyrosine kinase inhibitors (TKIs) targeting EGFR-mutant lung cancers promote a range of tumor regression responses to yield variable residual disease, a likely incubator for acquired resistance. Herein, rapid transcriptional responses induced by TKIs early in treatment that associate with the range of patient responses were explored. RNAseq was performed on EGFR mutant cell lines treated in vitro with osimertinib and on tumor biopsies of eight EGFR mutant lung cancer patients before and after 2 weeks of TKI treatment. Data were evaluated for gene expression programs altered upon TKI treatment. Chemokine and cytokine expression were measured by ELISA and quantitative RT-PCR. IκB Kinase (IKK) and JAK-STAT pathway dependence was tested with pharmacologic and molecular inhibitors. Tumor sections were stained for the T-cell marker CD3. Osimertinib stimulated dynamic, yet wide-ranging interferon (IFN) program regulation in EGFR mutant cell lines. IL6 and CXCL10 induction varied markedly among the EGFR mutant cell lines and was sensitive to IKK and JAK-STAT inhibitors. Analysis of matched patient biopsy pairs revealed marked, yet varied enrichment of IFN transcriptional programs, effector immune cell signatures and T-cell content in treated tumors that positively correlated with time to progression in the patients. EGFR-specific TKIs induce wide-ranging IFN response program activation originating within the cancer cell. The strong association of IFN program induction and duration of clinical response indicates that the TKI-induced IFN program instructs variable recruitment and participation of immune cells in the overall therapeutic response.https://doi.org/10.1038/s41698-021-00181-4
collection DOAJ
language English
format Article
sources DOAJ
author Natalia J. Gurule
Caroline E. McCoach
Trista K. Hinz
Daniel T. Merrick
Adriaan Van Bokhoven
Jihye Kim
Tejas Patil
Jacob Calhoun
Raphael A. Nemenoff
Aik Choon Tan
Robert C. Doebele
Lynn E. Heasley
spellingShingle Natalia J. Gurule
Caroline E. McCoach
Trista K. Hinz
Daniel T. Merrick
Adriaan Van Bokhoven
Jihye Kim
Tejas Patil
Jacob Calhoun
Raphael A. Nemenoff
Aik Choon Tan
Robert C. Doebele
Lynn E. Heasley
A tyrosine kinase inhibitor-induced interferon response positively associates with clinical response in EGFR-mutant lung cancer
npj Precision Oncology
author_facet Natalia J. Gurule
Caroline E. McCoach
Trista K. Hinz
Daniel T. Merrick
Adriaan Van Bokhoven
Jihye Kim
Tejas Patil
Jacob Calhoun
Raphael A. Nemenoff
Aik Choon Tan
Robert C. Doebele
Lynn E. Heasley
author_sort Natalia J. Gurule
title A tyrosine kinase inhibitor-induced interferon response positively associates with clinical response in EGFR-mutant lung cancer
title_short A tyrosine kinase inhibitor-induced interferon response positively associates with clinical response in EGFR-mutant lung cancer
title_full A tyrosine kinase inhibitor-induced interferon response positively associates with clinical response in EGFR-mutant lung cancer
title_fullStr A tyrosine kinase inhibitor-induced interferon response positively associates with clinical response in EGFR-mutant lung cancer
title_full_unstemmed A tyrosine kinase inhibitor-induced interferon response positively associates with clinical response in EGFR-mutant lung cancer
title_sort tyrosine kinase inhibitor-induced interferon response positively associates with clinical response in egfr-mutant lung cancer
publisher Nature Publishing Group
series npj Precision Oncology
issn 2397-768X
publishDate 2021-05-01
description Abstract Tyrosine kinase inhibitors (TKIs) targeting EGFR-mutant lung cancers promote a range of tumor regression responses to yield variable residual disease, a likely incubator for acquired resistance. Herein, rapid transcriptional responses induced by TKIs early in treatment that associate with the range of patient responses were explored. RNAseq was performed on EGFR mutant cell lines treated in vitro with osimertinib and on tumor biopsies of eight EGFR mutant lung cancer patients before and after 2 weeks of TKI treatment. Data were evaluated for gene expression programs altered upon TKI treatment. Chemokine and cytokine expression were measured by ELISA and quantitative RT-PCR. IκB Kinase (IKK) and JAK-STAT pathway dependence was tested with pharmacologic and molecular inhibitors. Tumor sections were stained for the T-cell marker CD3. Osimertinib stimulated dynamic, yet wide-ranging interferon (IFN) program regulation in EGFR mutant cell lines. IL6 and CXCL10 induction varied markedly among the EGFR mutant cell lines and was sensitive to IKK and JAK-STAT inhibitors. Analysis of matched patient biopsy pairs revealed marked, yet varied enrichment of IFN transcriptional programs, effector immune cell signatures and T-cell content in treated tumors that positively correlated with time to progression in the patients. EGFR-specific TKIs induce wide-ranging IFN response program activation originating within the cancer cell. The strong association of IFN program induction and duration of clinical response indicates that the TKI-induced IFN program instructs variable recruitment and participation of immune cells in the overall therapeutic response.
url https://doi.org/10.1038/s41698-021-00181-4
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