Mutation profiles in early-stage lung squamous cell carcinoma with clinical follow-up and correlation with markers of immune function

M. Choi; H. Kadara; J. Zhang; E. R. Parra; J. Rodriguez-Canales; S. G. Gaffney; Z. Zhao; C. Behrens; J. Fujimoto; C. Chow; K. Kim; N. Kalhor; C. Moran; D. Rimm; S. Swisher; D. L. Gibbons; J. Heymach; E. Kaftan; J. P. Townsend; T. J. Lynch; J. Schlessinger; J. Lee; R. P. Lifton; R. S. Herbst; I. I. Wistuba

doi:10.1093/annonc/mdw437

Mutation profiles in early-stage lung squamous cell carcinoma with clinical follow-up and correlation with markers of immune function

M. Choi, H. Kadara, J. Zhang, E. R. Parra, J. Rodriguez-Canales, S. G. Gaffney, Z. Zhao, C. Behrens, J. Fujimoto, C. Chow, K. Kim, N. Kalhor, C. Moran, D. Rimm, S. Swisher, D. L. Gibbons, J. Heymach, E. Kaftan, J. P. Townsend, T. J. LynchJ. Schlessinger, J. Lee, R. P. Lifton, R. S. Herbst, I. I. Wistuba

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

81 Scopus citations

Abstract

Background: Lung squamous cell carcinoma (LUSC) accounts for 20-30% of non-small cell lung cancers (NSCLCs). There are limited treatment strategies for LUSC in part due to our inadequate understanding of the molecular underpinnings of the disease. We performed whole-exome sequencing (WES) and comprehensive immune profiling of a unique set of clinically annotated early-stage LUSCs to increase our understanding of the pathobiology of this malignancy. Methods: Matched pairs of surgically resected stage I-III LUSCs and normal lung tissues (n=108) were analyzed by WES. Immunohistochemistry and image analysis-based profiling of 10 immune markers were done on a subset of LUSCs (n=91). Associations among mutations, immune markers and clinicopathological variables were statistically examined using analysis of variance and Fisher's exact test. Cox proportional hazards regression models were used for statistical analysis of clinical outcome. Results: This early-stage LUSC cohort displayed an average of 209 exonic mutations per tumor. Fourteen genes exhibited significant enrichment for somatic mutation: TP53, MLL2, PIK3CA, NFE2L2, CDH8, KEAP1, PTEN, ADCY8, PTPRT, CALCR, GRM8, FBXW7, RB1 and CDKN2A. Among mutated genes associated with poor recurrence-free survival, MLL2 mutations predicted poor prognosis in both TP53 mutant and wild-type LUSCs. We also found that in treated patients, FBXW7 and KEAP1 mutations were associated with poor response to adjuvant therapy, particularly in TP53-mutant tumors. Analysis of mutations with immune markers revealed that ADCY8 and PIK3CA mutations were associated with markedly decreased tumoral PD-L1 expression, LUSCs with PIK3CA mutations exhibited elevated CD45ro levels and CDKN2A-mutant tumors displayed an up-regulated immune response. Conclusion(s): Our findings pinpoint mutated genes that may impact clinical outcome as well as personalized strategies for targeted immunotherapies in early-stage LUSC.

Original language	English (US)
Pages (from-to)	83-89
Number of pages	7
Journal	Annals of Oncology
Volume	28
Issue number	1
DOIs	https://doi.org/10.1093/annonc/mdw437
State	Published - Jan 1 2017

Keywords

Immune profiles
LUSC
Whole exome sequencing

ASJC Scopus subject areas

Hematology
Oncology

MD Anderson CCSG core facilities

Biostatistics Resource Group

Access to Document

10.1093/annonc/mdw437

Cite this

Choi, M., Kadara, H., Zhang, J., Parra, E. R., Rodriguez-Canales, J., Gaffney, S. G., Zhao, Z., Behrens, C., Fujimoto, J., Chow, C., Kim, K., Kalhor, N., Moran, C., Rimm, D., Swisher, S., Gibbons, D. L., Heymach, J., Kaftan, E., Townsend, J. P., ... Wistuba, I. I. (2017). Mutation profiles in early-stage lung squamous cell carcinoma with clinical follow-up and correlation with markers of immune function. Annals of Oncology, 28(1), 83-89. https://doi.org/10.1093/annonc/mdw437

Choi, M, Kadara, H , Zhang, J , Parra, ER, Rodriguez-Canales, J, Gaffney, SG, Zhao, Z, Behrens, C, Fujimoto, J, Chow, C, Kim, K, Kalhor, N , Moran, C, Rimm, D, Swisher, S , Gibbons, DL , Heymach, J, Kaftan, E, Townsend, JP, Lynch, TJ, Schlessinger, J, Lee, J, Lifton, RP, Herbst, RS & Wistuba, II 2017, 'Mutation profiles in early-stage lung squamous cell carcinoma with clinical follow-up and correlation with markers of immune function', Annals of Oncology, vol. 28, no. 1, pp. 83-89. https://doi.org/10.1093/annonc/mdw437

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title = "Mutation profiles in early-stage lung squamous cell carcinoma with clinical follow-up and correlation with markers of immune function",

abstract = "Background: Lung squamous cell carcinoma (LUSC) accounts for 20-30% of non-small cell lung cancers (NSCLCs). There are limited treatment strategies for LUSC in part due to our inadequate understanding of the molecular underpinnings of the disease. We performed whole-exome sequencing (WES) and comprehensive immune profiling of a unique set of clinically annotated early-stage LUSCs to increase our understanding of the pathobiology of this malignancy. Methods: Matched pairs of surgically resected stage I-III LUSCs and normal lung tissues (n=108) were analyzed by WES. Immunohistochemistry and image analysis-based profiling of 10 immune markers were done on a subset of LUSCs (n=91). Associations among mutations, immune markers and clinicopathological variables were statistically examined using analysis of variance and Fisher's exact test. Cox proportional hazards regression models were used for statistical analysis of clinical outcome. Results: This early-stage LUSC cohort displayed an average of 209 exonic mutations per tumor. Fourteen genes exhibited significant enrichment for somatic mutation: TP53, MLL2, PIK3CA, NFE2L2, CDH8, KEAP1, PTEN, ADCY8, PTPRT, CALCR, GRM8, FBXW7, RB1 and CDKN2A. Among mutated genes associated with poor recurrence-free survival, MLL2 mutations predicted poor prognosis in both TP53 mutant and wild-type LUSCs. We also found that in treated patients, FBXW7 and KEAP1 mutations were associated with poor response to adjuvant therapy, particularly in TP53-mutant tumors. Analysis of mutations with immune markers revealed that ADCY8 and PIK3CA mutations were associated with markedly decreased tumoral PD-L1 expression, LUSCs with PIK3CA mutations exhibited elevated CD45ro levels and CDKN2A-mutant tumors displayed an up-regulated immune response. Conclusion(s): Our findings pinpoint mutated genes that may impact clinical outcome as well as personalized strategies for targeted immunotherapies in early-stage LUSC.",

keywords = "Immune profiles, LUSC, Whole exome sequencing",

author = "M. Choi and H. Kadara and J. Zhang and Parra, {E. R.} and J. Rodriguez-Canales and Gaffney, {S. G.} and Z. Zhao and C. Behrens and J. Fujimoto and C. Chow and K. Kim and N. Kalhor and C. Moran and D. Rimm and S. Swisher and Gibbons, {D. L.} and J. Heymach and E. Kaftan and Townsend, {J. P.} and Lynch, {T. J.} and J. Schlessinger and J. Lee and Lifton, {R. P.} and Herbst, {R. S.} and Wistuba, {I. I.}",

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doi = "10.1093/annonc/mdw437",

language = "English (US)",

volume = "28",

pages = "83--89",

journal = "Annals of Oncology",

issn = "0923-7534",

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TY - JOUR

T1 - Mutation profiles in early-stage lung squamous cell carcinoma with clinical follow-up and correlation with markers of immune function

AU - Choi, M.

AU - Kadara, H.

AU - Zhang, J.

AU - Parra, E. R.

AU - Rodriguez-Canales, J.

AU - Gaffney, S. G.

AU - Zhao, Z.

AU - Behrens, C.

AU - Fujimoto, J.

AU - Chow, C.

AU - Kim, K.

AU - Kalhor, N.

AU - Moran, C.

AU - Rimm, D.

AU - Swisher, S.

AU - Gibbons, D. L.

AU - Heymach, J.

AU - Kaftan, E.

AU - Townsend, J. P.

AU - Lynch, T. J.

AU - Schlessinger, J.

AU - Lee, J.

AU - Lifton, R. P.

AU - Herbst, R. S.

AU - Wistuba, I. I.

PY - 2017/1/1

Y1 - 2017/1/1

N2 - Background: Lung squamous cell carcinoma (LUSC) accounts for 20-30% of non-small cell lung cancers (NSCLCs). There are limited treatment strategies for LUSC in part due to our inadequate understanding of the molecular underpinnings of the disease. We performed whole-exome sequencing (WES) and comprehensive immune profiling of a unique set of clinically annotated early-stage LUSCs to increase our understanding of the pathobiology of this malignancy. Methods: Matched pairs of surgically resected stage I-III LUSCs and normal lung tissues (n=108) were analyzed by WES. Immunohistochemistry and image analysis-based profiling of 10 immune markers were done on a subset of LUSCs (n=91). Associations among mutations, immune markers and clinicopathological variables were statistically examined using analysis of variance and Fisher's exact test. Cox proportional hazards regression models were used for statistical analysis of clinical outcome. Results: This early-stage LUSC cohort displayed an average of 209 exonic mutations per tumor. Fourteen genes exhibited significant enrichment for somatic mutation: TP53, MLL2, PIK3CA, NFE2L2, CDH8, KEAP1, PTEN, ADCY8, PTPRT, CALCR, GRM8, FBXW7, RB1 and CDKN2A. Among mutated genes associated with poor recurrence-free survival, MLL2 mutations predicted poor prognosis in both TP53 mutant and wild-type LUSCs. We also found that in treated patients, FBXW7 and KEAP1 mutations were associated with poor response to adjuvant therapy, particularly in TP53-mutant tumors. Analysis of mutations with immune markers revealed that ADCY8 and PIK3CA mutations were associated with markedly decreased tumoral PD-L1 expression, LUSCs with PIK3CA mutations exhibited elevated CD45ro levels and CDKN2A-mutant tumors displayed an up-regulated immune response. Conclusion(s): Our findings pinpoint mutated genes that may impact clinical outcome as well as personalized strategies for targeted immunotherapies in early-stage LUSC.

AB - Background: Lung squamous cell carcinoma (LUSC) accounts for 20-30% of non-small cell lung cancers (NSCLCs). There are limited treatment strategies for LUSC in part due to our inadequate understanding of the molecular underpinnings of the disease. We performed whole-exome sequencing (WES) and comprehensive immune profiling of a unique set of clinically annotated early-stage LUSCs to increase our understanding of the pathobiology of this malignancy. Methods: Matched pairs of surgically resected stage I-III LUSCs and normal lung tissues (n=108) were analyzed by WES. Immunohistochemistry and image analysis-based profiling of 10 immune markers were done on a subset of LUSCs (n=91). Associations among mutations, immune markers and clinicopathological variables were statistically examined using analysis of variance and Fisher's exact test. Cox proportional hazards regression models were used for statistical analysis of clinical outcome. Results: This early-stage LUSC cohort displayed an average of 209 exonic mutations per tumor. Fourteen genes exhibited significant enrichment for somatic mutation: TP53, MLL2, PIK3CA, NFE2L2, CDH8, KEAP1, PTEN, ADCY8, PTPRT, CALCR, GRM8, FBXW7, RB1 and CDKN2A. Among mutated genes associated with poor recurrence-free survival, MLL2 mutations predicted poor prognosis in both TP53 mutant and wild-type LUSCs. We also found that in treated patients, FBXW7 and KEAP1 mutations were associated with poor response to adjuvant therapy, particularly in TP53-mutant tumors. Analysis of mutations with immune markers revealed that ADCY8 and PIK3CA mutations were associated with markedly decreased tumoral PD-L1 expression, LUSCs with PIK3CA mutations exhibited elevated CD45ro levels and CDKN2A-mutant tumors displayed an up-regulated immune response. Conclusion(s): Our findings pinpoint mutated genes that may impact clinical outcome as well as personalized strategies for targeted immunotherapies in early-stage LUSC.

KW - Immune profiles

KW - LUSC

KW - Whole exome sequencing

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Mutation profiles in early-stage lung squamous cell carcinoma with clinical follow-up and correlation with markers of immune function

Abstract

Keywords

ASJC Scopus subject areas

MD Anderson CCSG core facilities

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