Tumor-infiltrating lymphocytes in glioblastoma are associated with specific genomic alterations and related to transcriptional class

W. Caleb Rutledge; Jun Kong; Jingjing Gao; David A. Gutman; Lee A.D. Cooper; Christina Appin; Yuna Park; Lisa Scarpace; Tom Mikkelsen; Mark L. Cohen; Kenneth D. Aldape; Roger E. McLendon; Norman L. Lehman; C. Ryan Miller; Matthew J. Schniederjan; Cameron W. Brennan; Joel H. Saltz; Carlos S. Moreno; Daniel J. Brat

doi:10.1158/1078-0432.CCR-13-0551

Tumor-infiltrating lymphocytes in glioblastoma are associated with specific genomic alterations and related to transcriptional class

W. Caleb Rutledge
, Jun Kong
, Jingjing Gao
, David A. Gutman
, Lee A.D. Cooper
, Christina Appin
, Yuna Park
, Lisa Scarpace
, Tom Mikkelsen
, Mark L. Cohen
, Kenneth D. Aldape
, Roger E. McLendon
, Norman L. Lehman
, C. Ryan Miller
, Matthew J. Schniederjan
, Cameron W. Brennan
, Joel H. Saltz
, Carlos S. Moreno
, Daniel J. Brat

Biomedical Informatics

Emory University
Center for Comprehensive Informatics
Henry Ford Health System
Case Western Reserve University
University of Texas Health Science Center at Houston
Duke University
Ohio State University
University of North Carolina at Chapel Hill
Children's Healthcare of Atlanta
Memorial Sloan-Kettering Cancer Center

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

173 Scopus citations

Abstract

Purpose: Tumor-infiltrating lymphocytes (TIL) have prognostic significance in many cancers, yet their roles in glioblastoma have not been fully defined. We hypothesized that TILs in glioblastoma are associated with molecular alterations, histologies, and survival. Experimental Design: We used data from The Cancer Genome Atlas (TCGA) to investigate molecular, histologic, and clinical correlates of TILs in glioblastomas. Lymphocytes were categorized as absent, present, or abundant in histopathologic images from 171 TCGA glioblastomas. Associations were examined between lymphocytes and histologic features, mutations, copy number alterations, CpG island methylator phenotype, transcriptional class, and survival. Wevalidated histologic findings usingCD3Ggene expression. Results: Wefound a positive correlation between TILs and glioblastomas with gemistocytes, sarcomatous cells, epithelioid cells, and giant cells. Lymphocytes were enriched in the mesenchymal transcriptional class and strongly associated with mutations in NF1 and RB1. These mutations are frequent in the mesenchymal class and characteristic of gemistocytic, sarcomatous, epithelioid, and giant cell histologies. Conversely, TILs were rare in glioblastomas with small cells and oligodendroglioma components. Lymphocytes were depleted in the classical transcriptional class and in EGF receptor (EGFR)-amplified and homozygous PTEN-deleted glioblastomas. These alterations are characteristic of glioblastomas with small cells and glioblastomas of the classical transcriptional class. No association with survival was shown. Conclusions: TILs were enriched in glioblastomas of the mesenchymal class, strongly associated with mutations in NF1 and RB1 and typical of histologies characterized by these mutations. Conversely, TILs were depleted in the classical class, EGFR-amplified, and homozygous PTEN-deleted tumors and rare in histologies characterized by these alterations.

Original language	English
Pages (from-to)	4951-4960
Number of pages	10
Journal	Clinical Cancer Research
Volume	19
Issue number	18
DOIs	https://doi.org/10.1158/1078-0432.CCR-13-0551
State	Published - Sep 15 2013

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Caleb Rutledge, W., Kong, J., Gao, J., Gutman, D. A., Cooper, L. A. D., Appin, C., Park, Y., Scarpace, L., Mikkelsen, T., Cohen, M. L., Aldape, K. D., McLendon, R. E., Lehman, N. L., Miller, C. R., Schniederjan, M. J., Brennan, C. W., Saltz, J. H., Moreno, C. S., & Brat, D. J. (2013). Tumor-infiltrating lymphocytes in glioblastoma are associated with specific genomic alterations and related to transcriptional class. Clinical Cancer Research, 19(18), 4951-4960. https://doi.org/10.1158/1078-0432.CCR-13-0551

@article{50ae2eaaabe44a58b5af0760d4d7ec4a,

title = "Tumor-infiltrating lymphocytes in glioblastoma are associated with specific genomic alterations and related to transcriptional class",

abstract = "Purpose: Tumor-infiltrating lymphocytes (TIL) have prognostic significance in many cancers, yet their roles in glioblastoma have not been fully defined. We hypothesized that TILs in glioblastoma are associated with molecular alterations, histologies, and survival. Experimental Design: We used data from The Cancer Genome Atlas (TCGA) to investigate molecular, histologic, and clinical correlates of TILs in glioblastomas. Lymphocytes were categorized as absent, present, or abundant in histopathologic images from 171 TCGA glioblastomas. Associations were examined between lymphocytes and histologic features, mutations, copy number alterations, CpG island methylator phenotype, transcriptional class, and survival. Wevalidated histologic findings usingCD3Ggene expression. Results: Wefound a positive correlation between TILs and glioblastomas with gemistocytes, sarcomatous cells, epithelioid cells, and giant cells. Lymphocytes were enriched in the mesenchymal transcriptional class and strongly associated with mutations in NF1 and RB1. These mutations are frequent in the mesenchymal class and characteristic of gemistocytic, sarcomatous, epithelioid, and giant cell histologies. Conversely, TILs were rare in glioblastomas with small cells and oligodendroglioma components. Lymphocytes were depleted in the classical transcriptional class and in EGF receptor (EGFR)-amplified and homozygous PTEN-deleted glioblastomas. These alterations are characteristic of glioblastomas with small cells and glioblastomas of the classical transcriptional class. No association with survival was shown. Conclusions: TILs were enriched in glioblastomas of the mesenchymal class, strongly associated with mutations in NF1 and RB1 and typical of histologies characterized by these mutations. Conversely, TILs were depleted in the classical class, EGFR-amplified, and homozygous PTEN-deleted tumors and rare in histologies characterized by these alterations.",

author = "\{Caleb Rutledge\}, W. and Jun Kong and Jingjing Gao and Gutman, \{David A.\} and Cooper, \{Lee A.D.\} and Christina Appin and Yuna Park and Lisa Scarpace and Tom Mikkelsen and Cohen, \{Mark L.\} and Aldape, \{Kenneth D.\} and McLendon, \{Roger E.\} and Lehman, \{Norman L.\} and Miller, \{C. Ryan\} and Schniederjan, \{Matthew J.\} and Brennan, \{Cameron W.\} and Saltz, \{Joel H.\} and Moreno, \{Carlos S.\} and Brat, \{Daniel J.\}",

year = "2013",

month = sep,

day = "15",

doi = "10.1158/1078-0432.CCR-13-0551",

language = "English",

volume = "19",

pages = "4951--4960",

journal = "Clinical Cancer Research",

issn = "1078-0432",

number = "18",

}

Caleb Rutledge, W, Kong, J, Gao, J, Gutman, DA, Cooper, LAD, Appin, C, Park, Y, Scarpace, L, Mikkelsen, T, Cohen, ML, Aldape, KD, McLendon, RE, Lehman, NL, Miller, CR, Schniederjan, MJ, Brennan, CW, Saltz, JH, Moreno, CS & Brat, DJ 2013, 'Tumor-infiltrating lymphocytes in glioblastoma are associated with specific genomic alterations and related to transcriptional class', Clinical Cancer Research, vol. 19, no. 18, pp. 4951-4960. https://doi.org/10.1158/1078-0432.CCR-13-0551

TY - JOUR

T1 - Tumor-infiltrating lymphocytes in glioblastoma are associated with specific genomic alterations and related to transcriptional class

AU - Caleb Rutledge, W.

AU - Kong, Jun

AU - Gao, Jingjing

AU - Gutman, David A.

AU - Cooper, Lee A.D.

AU - Appin, Christina

AU - Park, Yuna

AU - Scarpace, Lisa

AU - Mikkelsen, Tom

AU - Cohen, Mark L.

AU - Aldape, Kenneth D.

AU - McLendon, Roger E.

AU - Lehman, Norman L.

AU - Miller, C. Ryan

AU - Schniederjan, Matthew J.

AU - Brennan, Cameron W.

AU - Saltz, Joel H.

AU - Moreno, Carlos S.

AU - Brat, Daniel J.

PY - 2013/9/15

Y1 - 2013/9/15

N2 - Purpose: Tumor-infiltrating lymphocytes (TIL) have prognostic significance in many cancers, yet their roles in glioblastoma have not been fully defined. We hypothesized that TILs in glioblastoma are associated with molecular alterations, histologies, and survival. Experimental Design: We used data from The Cancer Genome Atlas (TCGA) to investigate molecular, histologic, and clinical correlates of TILs in glioblastomas. Lymphocytes were categorized as absent, present, or abundant in histopathologic images from 171 TCGA glioblastomas. Associations were examined between lymphocytes and histologic features, mutations, copy number alterations, CpG island methylator phenotype, transcriptional class, and survival. Wevalidated histologic findings usingCD3Ggene expression. Results: Wefound a positive correlation between TILs and glioblastomas with gemistocytes, sarcomatous cells, epithelioid cells, and giant cells. Lymphocytes were enriched in the mesenchymal transcriptional class and strongly associated with mutations in NF1 and RB1. These mutations are frequent in the mesenchymal class and characteristic of gemistocytic, sarcomatous, epithelioid, and giant cell histologies. Conversely, TILs were rare in glioblastomas with small cells and oligodendroglioma components. Lymphocytes were depleted in the classical transcriptional class and in EGF receptor (EGFR)-amplified and homozygous PTEN-deleted glioblastomas. These alterations are characteristic of glioblastomas with small cells and glioblastomas of the classical transcriptional class. No association with survival was shown. Conclusions: TILs were enriched in glioblastomas of the mesenchymal class, strongly associated with mutations in NF1 and RB1 and typical of histologies characterized by these mutations. Conversely, TILs were depleted in the classical class, EGFR-amplified, and homozygous PTEN-deleted tumors and rare in histologies characterized by these alterations.

AB - Purpose: Tumor-infiltrating lymphocytes (TIL) have prognostic significance in many cancers, yet their roles in glioblastoma have not been fully defined. We hypothesized that TILs in glioblastoma are associated with molecular alterations, histologies, and survival. Experimental Design: We used data from The Cancer Genome Atlas (TCGA) to investigate molecular, histologic, and clinical correlates of TILs in glioblastomas. Lymphocytes were categorized as absent, present, or abundant in histopathologic images from 171 TCGA glioblastomas. Associations were examined between lymphocytes and histologic features, mutations, copy number alterations, CpG island methylator phenotype, transcriptional class, and survival. Wevalidated histologic findings usingCD3Ggene expression. Results: Wefound a positive correlation between TILs and glioblastomas with gemistocytes, sarcomatous cells, epithelioid cells, and giant cells. Lymphocytes were enriched in the mesenchymal transcriptional class and strongly associated with mutations in NF1 and RB1. These mutations are frequent in the mesenchymal class and characteristic of gemistocytic, sarcomatous, epithelioid, and giant cell histologies. Conversely, TILs were rare in glioblastomas with small cells and oligodendroglioma components. Lymphocytes were depleted in the classical transcriptional class and in EGF receptor (EGFR)-amplified and homozygous PTEN-deleted glioblastomas. These alterations are characteristic of glioblastomas with small cells and glioblastomas of the classical transcriptional class. No association with survival was shown. Conclusions: TILs were enriched in glioblastomas of the mesenchymal class, strongly associated with mutations in NF1 and RB1 and typical of histologies characterized by these mutations. Conversely, TILs were depleted in the classical class, EGFR-amplified, and homozygous PTEN-deleted tumors and rare in histologies characterized by these alterations.

UR - https://www.scopus.com/pages/publications/84884543901

U2 - 10.1158/1078-0432.CCR-13-0551

DO - 10.1158/1078-0432.CCR-13-0551

M3 - Article

C2 - 23864165

AN - SCOPUS:84884543901

SN - 1078-0432

VL - 19

SP - 4951

EP - 4960

JO - Clinical Cancer Research

JF - Clinical Cancer Research

IS - 18

ER -

Tumor-infiltrating lymphocytes in glioblastoma are associated with specific genomic alterations and related to transcriptional class

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