The Immune Landscape of Cancer

Cancer Genome Atlas Research Network

doi:10.1016/j.immuni.2019.08.004

The Immune Landscape of Cancer

Cancer Genome Atlas Research Network

Onderzoeksoutput: Bijdrage aan tijdschrift › Artikel › peer review

2843 Citaten (Scopus)

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We performed an extensive immunogenomic analysis of more than 10,000 tumors comprising 33 diverse cancer types by utilizing data compiled by TCGA. Across cancer types, we identified six immune subtypes—wound healing, IFN-γ dominant, inflammatory, lymphocyte depleted, immunologically quiet, and TGF-β dominant—characterized by differences in macrophage or lymphocyte signatures, Th1:Th2 cell ratio, extent of intratumoral heterogeneity, aneuploidy, extent of neoantigen load, overall cell proliferation, expression of immunomodulatory genes, and prognosis. Specific driver mutations correlated with lower (CTNNB1, NRAS, or IDH1) or higher (BRAF, TP53, or CASP8) leukocyte levels across all cancers. Multiple control modalities of the intracellular and extracellular networks (transcription, microRNAs, copy number, and epigenetic processes) were involved in tumor-immune cell interactions, both across and within immune subtypes. Our immunogenomics pipeline to characterize these heterogeneous tumors and the resulting data are intended to serve as a resource for future targeted studies to further advance the field. Thorsson et al. present immunogenomics analyses of more than 10,000 tumors, identifying six immune subtypes that encompass multiple cancer types and are hypothesized to define immune response patterns impacting prognosis. This work provides a resource for understanding tumor-immune interactions, with implications for identifying ways to advance research on immunotherapy.

Originele taal-2	Engels
Pagina's (van-tot)	411-412
Aantal pagina's	2
Tijdschrift	Immunity
Volume	51
Nummer van het tijdschrift	2
DOI's	https://doi.org/10.1016/j.immuni.2019.08.004 https://doi.org/10.1016/j.immuni.2018.03.023
Status	Gepubliceerd - 20 aug. 2019
Extern gepubliceerd	Ja

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title = "The Immune Landscape of Cancer",

abstract = "We performed an extensive immunogenomic analysis of more than 10,000 tumors comprising 33 diverse cancer types by utilizing data compiled by TCGA. Across cancer types, we identified six immune subtypes—wound healing, IFN-γ dominant, inflammatory, lymphocyte depleted, immunologically quiet, and TGF-β dominant—characterized by differences in macrophage or lymphocyte signatures, Th1:Th2 cell ratio, extent of intratumoral heterogeneity, aneuploidy, extent of neoantigen load, overall cell proliferation, expression of immunomodulatory genes, and prognosis. Specific driver mutations correlated with lower (CTNNB1, NRAS, or IDH1) or higher (BRAF, TP53, or CASP8) leukocyte levels across all cancers. Multiple control modalities of the intracellular and extracellular networks (transcription, microRNAs, copy number, and epigenetic processes) were involved in tumor-immune cell interactions, both across and within immune subtypes. Our immunogenomics pipeline to characterize these heterogeneous tumors and the resulting data are intended to serve as a resource for future targeted studies to further advance the field. Thorsson et al. present immunogenomics analyses of more than 10,000 tumors, identifying six immune subtypes that encompass multiple cancer types and are hypothesized to define immune response patterns impacting prognosis. This work provides a resource for understanding tumor-immune interactions, with implications for identifying ways to advance research on immunotherapy.",

keywords = "cancer genomics, immune subtypes, immuno-oncology, immunomodulatory, immunotherapy, integrative network analysis, tumor immunology, tumor microenvironment",

author = "{Cancer Genome Atlas Research Network} and V{\'e}steinn Thorsson and Gibbs, {David L} and Brown, {Scott D} and Denise Wolf and Bortone, {Dante S} and {Ou Yang}, Tai-Hsien and Eduard Porta-Pardo and Gao, {Galen F} and Plaisier, {Christopher L} and Eddy, {James A} and Elad Ziv and Culhane, {Aedin C} and Paull, {Evan O} and Sivakumar, {I K Ashok} and Gentles, {Andrew J} and Raunaq Malhotra and Farshad Farshidfar and Antonio Colaprico and Parker, {Joel S} and Mose, {Lisle E} and Vo, {Nam Sy} and Jianfang Liu and Yuexin Liu and Janet Rader and Varsha Dhankani and Reynolds, {Sheila M} and Reanne Bowlby and Andrea Califano and Cherniack, {Andrew D} and Dimitris Anastassiou and Davide Bedognetti and Younes Mokrab and Newman, {Aaron M} and Arvind Rao and Ken Chen and Alexander Krasnitz and Hai Hu and Malta, {Tathiane M} and Houtan Noushmehr and Pedamallu, {Chandra Sekhar} and Susan Bullman and Ojesina, {Akinyemi I} and Andrew Lamb and Wanding Zhou and Hui Shen and Choueiri, {Toni K} and Weinstein, {John N} and Justin Guinney and Joel Saltz and Holt, {Robert A}",

note = "Publisher Copyright: {\textcopyright} 2018 The Authors",

year = "2019",

month = aug,

day = "20",

doi = "10.1016/j.immuni.2019.08.004",

language = "English",

volume = "51",

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journal = "Immunity",

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T1 - The Immune Landscape of Cancer

AU - Cancer Genome Atlas Research Network

AU - Thorsson, Vésteinn

AU - Gibbs, David L

AU - Brown, Scott D

AU - Wolf, Denise

AU - Bortone, Dante S

AU - Ou Yang, Tai-Hsien

AU - Porta-Pardo, Eduard

AU - Gao, Galen F

AU - Plaisier, Christopher L

AU - Eddy, James A

AU - Ziv, Elad

AU - Culhane, Aedin C

AU - Paull, Evan O

AU - Sivakumar, I K Ashok

AU - Gentles, Andrew J

AU - Malhotra, Raunaq

AU - Farshidfar, Farshad

AU - Colaprico, Antonio

AU - Parker, Joel S

AU - Mose, Lisle E

AU - Vo, Nam Sy

AU - Liu, Jianfang

AU - Liu, Yuexin

AU - Rader, Janet

AU - Dhankani, Varsha

AU - Reynolds, Sheila M

AU - Bowlby, Reanne

AU - Califano, Andrea

AU - Cherniack, Andrew D

AU - Anastassiou, Dimitris

AU - Bedognetti, Davide

AU - Mokrab, Younes

AU - Newman, Aaron M

AU - Rao, Arvind

AU - Chen, Ken

AU - Krasnitz, Alexander

AU - Hu, Hai

AU - Malta, Tathiane M

AU - Noushmehr, Houtan

AU - Pedamallu, Chandra Sekhar

AU - Bullman, Susan

AU - Ojesina, Akinyemi I

AU - Lamb, Andrew

AU - Zhou, Wanding

AU - Shen, Hui

AU - Choueiri, Toni K

AU - Weinstein, John N

AU - Guinney, Justin

AU - Saltz, Joel

AU - Holt, Robert A

PY - 2019/8/20

Y1 - 2019/8/20

N2 - We performed an extensive immunogenomic analysis of more than 10,000 tumors comprising 33 diverse cancer types by utilizing data compiled by TCGA. Across cancer types, we identified six immune subtypes—wound healing, IFN-γ dominant, inflammatory, lymphocyte depleted, immunologically quiet, and TGF-β dominant—characterized by differences in macrophage or lymphocyte signatures, Th1:Th2 cell ratio, extent of intratumoral heterogeneity, aneuploidy, extent of neoantigen load, overall cell proliferation, expression of immunomodulatory genes, and prognosis. Specific driver mutations correlated with lower (CTNNB1, NRAS, or IDH1) or higher (BRAF, TP53, or CASP8) leukocyte levels across all cancers. Multiple control modalities of the intracellular and extracellular networks (transcription, microRNAs, copy number, and epigenetic processes) were involved in tumor-immune cell interactions, both across and within immune subtypes. Our immunogenomics pipeline to characterize these heterogeneous tumors and the resulting data are intended to serve as a resource for future targeted studies to further advance the field. Thorsson et al. present immunogenomics analyses of more than 10,000 tumors, identifying six immune subtypes that encompass multiple cancer types and are hypothesized to define immune response patterns impacting prognosis. This work provides a resource for understanding tumor-immune interactions, with implications for identifying ways to advance research on immunotherapy.

AB - We performed an extensive immunogenomic analysis of more than 10,000 tumors comprising 33 diverse cancer types by utilizing data compiled by TCGA. Across cancer types, we identified six immune subtypes—wound healing, IFN-γ dominant, inflammatory, lymphocyte depleted, immunologically quiet, and TGF-β dominant—characterized by differences in macrophage or lymphocyte signatures, Th1:Th2 cell ratio, extent of intratumoral heterogeneity, aneuploidy, extent of neoantigen load, overall cell proliferation, expression of immunomodulatory genes, and prognosis. Specific driver mutations correlated with lower (CTNNB1, NRAS, or IDH1) or higher (BRAF, TP53, or CASP8) leukocyte levels across all cancers. Multiple control modalities of the intracellular and extracellular networks (transcription, microRNAs, copy number, and epigenetic processes) were involved in tumor-immune cell interactions, both across and within immune subtypes. Our immunogenomics pipeline to characterize these heterogeneous tumors and the resulting data are intended to serve as a resource for future targeted studies to further advance the field. Thorsson et al. present immunogenomics analyses of more than 10,000 tumors, identifying six immune subtypes that encompass multiple cancer types and are hypothesized to define immune response patterns impacting prognosis. This work provides a resource for understanding tumor-immune interactions, with implications for identifying ways to advance research on immunotherapy.

KW - cancer genomics

KW - immune subtypes

KW - immuno-oncology

KW - immunomodulatory

KW - immunotherapy

KW - integrative network analysis

KW - tumor immunology

KW - tumor microenvironment

UR - http://www.scopus.com/inward/record.url?scp=85044934017&partnerID=8YFLogxK

U2 - 10.1016/j.immuni.2019.08.004

DO - 10.1016/j.immuni.2019.08.004

M3 - Article

C2 - 31433971

SN - 1074-7613

VL - 51

SP - 411

EP - 412

JO - Immunity

JF - Immunity

IS - 2

ER -

The Immune Landscape of Cancer

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