Co-clinical trials demonstrate predictive biomarkers for dovitinib, an FGFR inhibitor, in lung squamous cell carcinoma

H. R. Kim; H. N. Kang; H. S. Shim; E. Y. Kim; J. Kim; D. J. Kim; J. G. Lee; C. Y. Lee; M. H. Hong; S. M. Kim; H. Kim; K. H. Pyo; M. R. Yun; H. J. Park; J. Y. Han; H. A. Youn; M. J. Ahn; S. Paik; T. M. Kim; B. C. Cho

doi:10.1093/annonc/mdx098

Co-clinical trials demonstrate predictive biomarkers for dovitinib, an FGFR inhibitor, in lung squamous cell carcinoma

H. R. Kim, H. N. Kang, H. S. Shim, E. Y. Kim, J. Kim, D. J. Kim, J. G. Lee, C. Y. Lee, M. H. Hong, S. M. Kim, H. Kim, K. H. Pyo, M. R. Yun, H. J. Park, J. Y. Han, H. A. Youn, M. J. Ahn, S. Paik, T. M. Kim, B. C. Cho

Department of Internal Medicine

Research output: Contribution to journal › Article › peer-review

42 Citations (Scopus)

Abstract

Background: We conducted co-clinical trials in patient-derived xenograft (PDX) models to identify predictive biomarkers for the multikinase inhibitor dovitinib in lung squamous cell carcinoma (LSCC). Methods: The PDX01-02 were established from LSCC patients enrolled in the phase II trial of dovitinib (NCT01861197) and PDX03-05 were established from LSCC patients receiving surgery. These five PDX tumors were subjected to in vivo test of dovitinib efficacy, whole exome sequencing and gene expression profiling. Results: The PDX tumors recapitulate histopathological properties and maintain genomic characteristics of originating tumors. Concordant with clinical outcomes of the trial enrolled-LSCC patients, dovitinib produced substantial tumor regression in PDX-01 and PDX-05, whereas it resulted in tumor progression in PDX-02. PDX-03 and -04 also displayed poor antitumor efficacy to dovitinib. Mutational and genome-wide copy number profiles revealed no correlation between genomic alterations of FGFR1-3 and sensitivity to dovitinib. Of note, gene expression profiles revealed differentially expressed genes including FGF3 and FGF19 between PDX-01 and 05 and PDX-02-04. Pathway analysis identified two FGFR signaling-related gene sets, FGFR ligand binding/activation and SHCmediated cascade pathway were substantially up-regulated in PDX-01 and 05, compared with PDX-02-04. The comparison of gene expression profiles between dovitinib-sensitive versus -resistant lung cancer cell lines in the Cancer Cell Line Encyclopedia database also found that transcriptional activation of 18 key signaling components in FGFR pathways can predict the sensitivity to dovitinib both in cell lines and PDX tumors. These results highlight FGFR pathway activation as a key molecular determinant for sensitivity to dovitinib. Conclusions: FGFR gene expression signatures are predictors for the response to dovitinib in LSCC.

Original language	English
Pages (from-to)	1250-1259
Number of pages	10
Journal	Annals of Oncology
Volume	28
Issue number	6
DOIs	https://doi.org/10.1093/annonc/mdx098
Publication status	Published - 2017 Jun 1

Bibliographical note

Publisher Copyright:
© The Author 2017. Published by Oxford University Press on behalf of the European Society for Medical Oncology. All rights reserved.

All Science Journal Classification (ASJC) codes

Hematology
Oncology

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1093/annonc/mdx098

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Kim, H. R., Kang, H. N., Shim, H. S., Kim, E. Y., Kim, J., Kim, D. J., Lee, J. G., Lee, C. Y., Hong, M. H., Kim, S. M., Kim, H., Pyo, K. H., Yun, M. R., Park, H. J., Han, J. Y., Youn, H. A., Ahn, M. J., Paik, S., Kim, T. M., & Cho, B. C. (2017). Co-clinical trials demonstrate predictive biomarkers for dovitinib, an FGFR inhibitor, in lung squamous cell carcinoma. Annals of Oncology, 28(6), 1250-1259. https://doi.org/10.1093/annonc/mdx098

@article{b845be7bdc0f4e8b8e14edd15ad0167e,

title = "Co-clinical trials demonstrate predictive biomarkers for dovitinib, an FGFR inhibitor, in lung squamous cell carcinoma",

abstract = "Background: We conducted co-clinical trials in patient-derived xenograft (PDX) models to identify predictive biomarkers for the multikinase inhibitor dovitinib in lung squamous cell carcinoma (LSCC). Methods: The PDX01-02 were established from LSCC patients enrolled in the phase II trial of dovitinib (NCT01861197) and PDX03-05 were established from LSCC patients receiving surgery. These five PDX tumors were subjected to in vivo test of dovitinib efficacy, whole exome sequencing and gene expression profiling. Results: The PDX tumors recapitulate histopathological properties and maintain genomic characteristics of originating tumors. Concordant with clinical outcomes of the trial enrolled-LSCC patients, dovitinib produced substantial tumor regression in PDX-01 and PDX-05, whereas it resulted in tumor progression in PDX-02. PDX-03 and -04 also displayed poor antitumor efficacy to dovitinib. Mutational and genome-wide copy number profiles revealed no correlation between genomic alterations of FGFR1-3 and sensitivity to dovitinib. Of note, gene expression profiles revealed differentially expressed genes including FGF3 and FGF19 between PDX-01 and 05 and PDX-02-04. Pathway analysis identified two FGFR signaling-related gene sets, FGFR ligand binding/activation and SHCmediated cascade pathway were substantially up-regulated in PDX-01 and 05, compared with PDX-02-04. The comparison of gene expression profiles between dovitinib-sensitive versus -resistant lung cancer cell lines in the Cancer Cell Line Encyclopedia database also found that transcriptional activation of 18 key signaling components in FGFR pathways can predict the sensitivity to dovitinib both in cell lines and PDX tumors. These results highlight FGFR pathway activation as a key molecular determinant for sensitivity to dovitinib. Conclusions: FGFR gene expression signatures are predictors for the response to dovitinib in LSCC.",

author = "Kim, {H. R.} and Kang, {H. N.} and Shim, {H. S.} and Kim, {E. Y.} and J. Kim and Kim, {D. J.} and Lee, {J. G.} and Lee, {C. Y.} and Hong, {M. H.} and Kim, {S. M.} and H. Kim and Pyo, {K. H.} and Yun, {M. R.} and Park, {H. J.} and Han, {J. Y.} and Youn, {H. A.} and Ahn, {M. J.} and S. Paik and Kim, {T. M.} and Cho, {B. C.}",

year = "2017",

month = jun,

day = "1",

doi = "10.1093/annonc/mdx098",

language = "English",

volume = "28",

pages = "1250--1259",

journal = "Annals of Oncology",

issn = "0923-7534",

publisher = "Oxford University Press",

number = "6",

}

Kim, HR, Kang, HN, Shim, HS, Kim, EY, Kim, J, Kim, DJ, Lee, JG, Lee, CY, Hong, MH, Kim, SM, Kim, H, Pyo, KH, Yun, MR, Park, HJ, Han, JY, Youn, HA, Ahn, MJ, Paik, S, Kim, TM & Cho, BC 2017, 'Co-clinical trials demonstrate predictive biomarkers for dovitinib, an FGFR inhibitor, in lung squamous cell carcinoma', Annals of Oncology, vol. 28, no. 6, pp. 1250-1259. https://doi.org/10.1093/annonc/mdx098

TY - JOUR

T1 - Co-clinical trials demonstrate predictive biomarkers for dovitinib, an FGFR inhibitor, in lung squamous cell carcinoma

AU - Kim, H. R.

AU - Kang, H. N.

AU - Shim, H. S.

AU - Kim, E. Y.

AU - Kim, J.

AU - Kim, D. J.

AU - Lee, J. G.

AU - Lee, C. Y.

AU - Hong, M. H.

AU - Kim, S. M.

AU - Kim, H.

AU - Pyo, K. H.

AU - Yun, M. R.

AU - Park, H. J.

AU - Han, J. Y.

AU - Youn, H. A.

AU - Ahn, M. J.

AU - Paik, S.

AU - Kim, T. M.

AU - Cho, B. C.

PY - 2017/6/1

Y1 - 2017/6/1

N2 - Background: We conducted co-clinical trials in patient-derived xenograft (PDX) models to identify predictive biomarkers for the multikinase inhibitor dovitinib in lung squamous cell carcinoma (LSCC). Methods: The PDX01-02 were established from LSCC patients enrolled in the phase II trial of dovitinib (NCT01861197) and PDX03-05 were established from LSCC patients receiving surgery. These five PDX tumors were subjected to in vivo test of dovitinib efficacy, whole exome sequencing and gene expression profiling. Results: The PDX tumors recapitulate histopathological properties and maintain genomic characteristics of originating tumors. Concordant with clinical outcomes of the trial enrolled-LSCC patients, dovitinib produced substantial tumor regression in PDX-01 and PDX-05, whereas it resulted in tumor progression in PDX-02. PDX-03 and -04 also displayed poor antitumor efficacy to dovitinib. Mutational and genome-wide copy number profiles revealed no correlation between genomic alterations of FGFR1-3 and sensitivity to dovitinib. Of note, gene expression profiles revealed differentially expressed genes including FGF3 and FGF19 between PDX-01 and 05 and PDX-02-04. Pathway analysis identified two FGFR signaling-related gene sets, FGFR ligand binding/activation and SHCmediated cascade pathway were substantially up-regulated in PDX-01 and 05, compared with PDX-02-04. The comparison of gene expression profiles between dovitinib-sensitive versus -resistant lung cancer cell lines in the Cancer Cell Line Encyclopedia database also found that transcriptional activation of 18 key signaling components in FGFR pathways can predict the sensitivity to dovitinib both in cell lines and PDX tumors. These results highlight FGFR pathway activation as a key molecular determinant for sensitivity to dovitinib. Conclusions: FGFR gene expression signatures are predictors for the response to dovitinib in LSCC.

AB - Background: We conducted co-clinical trials in patient-derived xenograft (PDX) models to identify predictive biomarkers for the multikinase inhibitor dovitinib in lung squamous cell carcinoma (LSCC). Methods: The PDX01-02 were established from LSCC patients enrolled in the phase II trial of dovitinib (NCT01861197) and PDX03-05 were established from LSCC patients receiving surgery. These five PDX tumors were subjected to in vivo test of dovitinib efficacy, whole exome sequencing and gene expression profiling. Results: The PDX tumors recapitulate histopathological properties and maintain genomic characteristics of originating tumors. Concordant with clinical outcomes of the trial enrolled-LSCC patients, dovitinib produced substantial tumor regression in PDX-01 and PDX-05, whereas it resulted in tumor progression in PDX-02. PDX-03 and -04 also displayed poor antitumor efficacy to dovitinib. Mutational and genome-wide copy number profiles revealed no correlation between genomic alterations of FGFR1-3 and sensitivity to dovitinib. Of note, gene expression profiles revealed differentially expressed genes including FGF3 and FGF19 between PDX-01 and 05 and PDX-02-04. Pathway analysis identified two FGFR signaling-related gene sets, FGFR ligand binding/activation and SHCmediated cascade pathway were substantially up-regulated in PDX-01 and 05, compared with PDX-02-04. The comparison of gene expression profiles between dovitinib-sensitive versus -resistant lung cancer cell lines in the Cancer Cell Line Encyclopedia database also found that transcriptional activation of 18 key signaling components in FGFR pathways can predict the sensitivity to dovitinib both in cell lines and PDX tumors. These results highlight FGFR pathway activation as a key molecular determinant for sensitivity to dovitinib. Conclusions: FGFR gene expression signatures are predictors for the response to dovitinib in LSCC.

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U2 - 10.1093/annonc/mdx098

DO - 10.1093/annonc/mdx098

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SN - 0923-7534

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EP - 1259

JO - Annals of Oncology

JF - Annals of Oncology

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ER -

Co-clinical trials demonstrate predictive biomarkers for dovitinib, an FGFR inhibitor, in lung squamous cell carcinoma

Abstract

Bibliographical note

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UN SDGs

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