Integrated genomic characterization of the human immunome in cancer

Yongsheng Li; Brandon Burgman; Daniel J. McGrail; Ming Sun; Dan Qi; Sachet A. Shukla; Erxi Wu; Anna Capasso; Shiaw Yih Lin; Catherine J. Wu; S. Gail Eckhardt; Gordon B. Mills; Bo Li; Nidhi Sahni; S. Stephen Yi

doi:10.1158/0008-5472.CAN-20-0384

Integrated genomic characterization of the human immunome in cancer

Yongsheng Li, Brandon Burgman, Daniel J. McGrail, Ming Sun, Dan Qi, Sachet A. Shukla, Erxi Wu, Anna Capasso, Shiaw Yih Lin, Catherine J. Wu, S. Gail Eckhardt, Gordon B. Mills, Bo Li, Nidhi Sahni, S. Stephen Yi

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

11 Scopus citations

Abstract

Alterations in immune-related pathways are common hallmarks of cancer. A comprehensive understanding of how cancer mutations rewire immune signaling networks and functional output across cancer types is instrumental to realize the full potential of immunotherapy. Here, we systematically interrogated somatic mutations involved in immune signaling that alter immune responses in patients with cancer. To do so, we developed a Network-based Integrative model to Prioritize Potential immune respondER genes (NIPPER). Identified mutations were enriched in essential protein domains and genes identified by NIPPER were associated with responsiveness to multiple immunotherapy modalities. These genes were used to devise an interactome network propagation framework integrated with drug-associated gene signatures to identify potential immunomodulatory drug candidates. Together, our systems-level analysis results help interpret the heterogeneous immune responses among patients and serve as a resource for future functional studies and targeted therapeutics.

Original language	English (US)
Pages (from-to)	4854-4867
Number of pages	14
Journal	Cancer research
Volume	80
Issue number	21
DOIs	https://doi.org/10.1158/0008-5472.CAN-20-0384
State	Published - Nov 1 2020

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1158/0008-5472.CAN-20-0384

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@article{ef3dc4743bef49f289d36e8fea5b1263,

title = "Integrated genomic characterization of the human immunome in cancer",

abstract = "Alterations in immune-related pathways are common hallmarks of cancer. A comprehensive understanding of how cancer mutations rewire immune signaling networks and functional output across cancer types is instrumental to realize the full potential of immunotherapy. Here, we systematically interrogated somatic mutations involved in immune signaling that alter immune responses in patients with cancer. To do so, we developed a Network-based Integrative model to Prioritize Potential immune respondER genes (NIPPER). Identified mutations were enriched in essential protein domains and genes identified by NIPPER were associated with responsiveness to multiple immunotherapy modalities. These genes were used to devise an interactome network propagation framework integrated with drug-associated gene signatures to identify potential immunomodulatory drug candidates. Together, our systems-level analysis results help interpret the heterogeneous immune responses among patients and serve as a resource for future functional studies and targeted therapeutics.",

author = "Yongsheng Li and Brandon Burgman and McGrail, {Daniel J.} and Ming Sun and Dan Qi and Shukla, {Sachet A.} and Erxi Wu and Anna Capasso and Lin, {Shiaw Yih} and Wu, {Catherine J.} and {Gail Eckhardt}, S. and Mills, {Gordon B.} and Bo Li and Nidhi Sahni and {Stephen Yi}, S.",

note = "Funding Information: The authors would like to acknowledge Kevin Drew and Edward M. Marcotte from University of Texas at Austin for helpful discussions. The authors are grateful to contributions from TCGA Research Network Analysis Working Group, and also acknowledge the Biomedical Research Computing Facility at UT Austin and Texas Advanced Computing Center (TACC) for high-performance computing assistance. This work was supported by NIH grant (K22CA214765 to S.S. Yi), Komen Foundation grant (CCR19609287 to S.S. Yi), Young Investigator Grant by Breast Cancer Alliance (to N. Sahni), Liz Tilberis Early Career Award by Ovarian Cancer Research Alliance (Grant# 649968 to N. Sahni), Alfred P. Sloan Scholar Research Fellowship (FG-2018-10723 to N. Sahni), Cancer Prevention and Research Institute of Texas grants RR170079 (to B. Li) and RR160093 (to S.G. Eckhardt). N. Sahni is a CPRIT Scholar in Cancer Research with funding from the Cancer Prevention and Research Institute of Texas (CPRIT) New Investigator Grant RR160021. D.J. McGrail is supported by NCI grant K99CA240689. S.A. Shukla acknowledges support from the NCI (R50RCA211482). A. Capasso is supported by Department of Defense grant CA191245. C.J. Wu is a Scholar of the Leukemia and Lymphoma Society. G.B. Mills is supported by a kind gift from the Miriam and Sheldon Adelson Medical Research Foundation, SAC110052 from the Susan G Komen Research Foundation, Breast Cancer Research Foundation, Ovarian Cancer Research Alliance, Prospect Creek Foundation, and NCI grant (U01CA217842). Funding Information: The authors would like to acknowledge Kevin Drew and Edward M. Marcotte from University of Texas at Austin for helpful discussions. The authors are grateful to contributions from TCGA Research Network Analysis Working Group, and also acknowledge the Biomedical Research Computing Facility at UT Austin and Texas Advanced Computing Center (TACC) for high-performance computing assistance. This work was supported by NIH grant (K22CA214765 to S.S. Yi), Komen Foundation grant (CCR19609287 to S.S. Yi), Young Investigator Grant by Breast Cancer Alliance (to N. Sahni), Liz Tilberis Early Career Award by Ovarian Cancer Research Alliance (Grant# 649968 to N. Sahni), Alfred P. Sloan Scholar Research Fellowship (FG-2018–10723 to N. Sahni), Cancer Prevention and Research Institute of Texas grants RR170079 (to B. Li) and RR160093 (to S.G. Eckhardt). N. Sahni is a CPRIT Scholar in Cancer Research with funding from the Cancer Prevention and Research Institute of Texas (CPRIT) New Investigator Grant RR160021. D.J. McGrail is supported by NCI grant K99CA240689. S.A. Shukla acknowledges support from the NCI (R50RCA211482). A. Capasso is supported by Department of Defense grant CA191245. C.J. Wu is a Scholar of the Leukemia and Lymphoma Society. G.B. Mills is supported by a kind gift from the Miriam and Sheldon Adelson Medical Research Foundation, SAC110052 from the Susan G Komen Research Foundation, Breast Cancer Research Foundation, Ovarian Cancer Research Alliance, Prospect Creek Foundation, and NCI grant (U01CA217842). Funding Information: D.J. McGrail reports grants from NCI (NCI grant K99CA240689) during the conduct of the study. S.A. Shukla reports grants from NCI during the conduct of the study, nonfinancial support and other compensation from Bristol-Myers Squibb (equity), personal fees from Neon Therapeutics (consulting), other compensation from Agenus Inc. (equity), Agios Pharmaceuticals (equity), Break-Bio Corp (equity), and Lumos Pharma (equity) outside the submitted work. C.J. Wu reports other from Neon Therapeutics (founder and SAB member) outside the submitted work, as well as a patent for PCT/US2011/036665 licensed to Neon Therapeutics. G.B. Mills reports personal fees, nonfinancial support, and other compensation from AstraZeneca (clinical trials support), personal fees and nonfinancial support from Chrysalis, personal fees, nonfinancial support, and other compensation from ImmunoMet (stock), personal fees and nonfinancial support from Ionis, personal fees, nonfinancial support, and other compensation from Lilly (clinical trials support), personal fees and nonfinancial support from PDX Pharma, personal fees, nonfinancial support, and other compensation from Signalchem (stock), personal fees and nonfinancial support from Symphogen, personal fees, nonfinancial support, and other compensation from Tarveda (stock), personal fees and nonfinancial support from Turbine and Zentalis, other compensation from Catena (stock), Genentech (clinical trials support), GSK (clinical trials support), grants from Adelson Medical Research Foundation, Breast Cancer Research Foundation, Komen Research Foundation, Ovarian Cancer Research Foundation, and Prospect Creek Foundation during the conduct of the study. N. Sahni reports grants from Breast Cancer Alliance, Ovarian Cancer Research Alliance, Alfred P. Sloan Foundation, and Cancer Prevention and Research Institute of Texas during the conduct of the study. S. Yi reports grants from Susan Komen Foundation and grants from NCI during the conduct of the study. No potential conflicts of interest were disclosed by the other authors. Publisher Copyright: {\textcopyright} 2020 American Association for Cancer Research.",

year = "2020",

month = nov,

day = "1",

doi = "10.1158/0008-5472.CAN-20-0384",

language = "English (US)",

volume = "80",

pages = "4854--4867",

journal = "Cancer research",

issn = "0008-5472",

publisher = "American Association for Cancer Research Inc.",

number = "21",

}

TY - JOUR

T1 - Integrated genomic characterization of the human immunome in cancer

AU - Li, Yongsheng

AU - Burgman, Brandon

AU - McGrail, Daniel J.

AU - Sun, Ming

AU - Qi, Dan

AU - Shukla, Sachet A.

AU - Wu, Erxi

AU - Capasso, Anna

AU - Lin, Shiaw Yih

AU - Wu, Catherine J.

AU - Gail Eckhardt, S.

AU - Mills, Gordon B.

AU - Li, Bo

AU - Sahni, Nidhi

AU - Stephen Yi, S.

N1 - Funding Information: The authors would like to acknowledge Kevin Drew and Edward M. Marcotte from University of Texas at Austin for helpful discussions. The authors are grateful to contributions from TCGA Research Network Analysis Working Group, and also acknowledge the Biomedical Research Computing Facility at UT Austin and Texas Advanced Computing Center (TACC) for high-performance computing assistance. This work was supported by NIH grant (K22CA214765 to S.S. Yi), Komen Foundation grant (CCR19609287 to S.S. Yi), Young Investigator Grant by Breast Cancer Alliance (to N. Sahni), Liz Tilberis Early Career Award by Ovarian Cancer Research Alliance (Grant# 649968 to N. Sahni), Alfred P. Sloan Scholar Research Fellowship (FG-2018-10723 to N. Sahni), Cancer Prevention and Research Institute of Texas grants RR170079 (to B. Li) and RR160093 (to S.G. Eckhardt). N. Sahni is a CPRIT Scholar in Cancer Research with funding from the Cancer Prevention and Research Institute of Texas (CPRIT) New Investigator Grant RR160021. D.J. McGrail is supported by NCI grant K99CA240689. S.A. Shukla acknowledges support from the NCI (R50RCA211482). A. Capasso is supported by Department of Defense grant CA191245. C.J. Wu is a Scholar of the Leukemia and Lymphoma Society. G.B. Mills is supported by a kind gift from the Miriam and Sheldon Adelson Medical Research Foundation, SAC110052 from the Susan G Komen Research Foundation, Breast Cancer Research Foundation, Ovarian Cancer Research Alliance, Prospect Creek Foundation, and NCI grant (U01CA217842). Funding Information: The authors would like to acknowledge Kevin Drew and Edward M. Marcotte from University of Texas at Austin for helpful discussions. The authors are grateful to contributions from TCGA Research Network Analysis Working Group, and also acknowledge the Biomedical Research Computing Facility at UT Austin and Texas Advanced Computing Center (TACC) for high-performance computing assistance. This work was supported by NIH grant (K22CA214765 to S.S. Yi), Komen Foundation grant (CCR19609287 to S.S. Yi), Young Investigator Grant by Breast Cancer Alliance (to N. Sahni), Liz Tilberis Early Career Award by Ovarian Cancer Research Alliance (Grant# 649968 to N. Sahni), Alfred P. Sloan Scholar Research Fellowship (FG-2018–10723 to N. Sahni), Cancer Prevention and Research Institute of Texas grants RR170079 (to B. Li) and RR160093 (to S.G. Eckhardt). N. Sahni is a CPRIT Scholar in Cancer Research with funding from the Cancer Prevention and Research Institute of Texas (CPRIT) New Investigator Grant RR160021. D.J. McGrail is supported by NCI grant K99CA240689. S.A. Shukla acknowledges support from the NCI (R50RCA211482). A. Capasso is supported by Department of Defense grant CA191245. C.J. Wu is a Scholar of the Leukemia and Lymphoma Society. G.B. Mills is supported by a kind gift from the Miriam and Sheldon Adelson Medical Research Foundation, SAC110052 from the Susan G Komen Research Foundation, Breast Cancer Research Foundation, Ovarian Cancer Research Alliance, Prospect Creek Foundation, and NCI grant (U01CA217842). Funding Information: D.J. McGrail reports grants from NCI (NCI grant K99CA240689) during the conduct of the study. S.A. Shukla reports grants from NCI during the conduct of the study, nonfinancial support and other compensation from Bristol-Myers Squibb (equity), personal fees from Neon Therapeutics (consulting), other compensation from Agenus Inc. (equity), Agios Pharmaceuticals (equity), Break-Bio Corp (equity), and Lumos Pharma (equity) outside the submitted work. C.J. Wu reports other from Neon Therapeutics (founder and SAB member) outside the submitted work, as well as a patent for PCT/US2011/036665 licensed to Neon Therapeutics. G.B. Mills reports personal fees, nonfinancial support, and other compensation from AstraZeneca (clinical trials support), personal fees and nonfinancial support from Chrysalis, personal fees, nonfinancial support, and other compensation from ImmunoMet (stock), personal fees and nonfinancial support from Ionis, personal fees, nonfinancial support, and other compensation from Lilly (clinical trials support), personal fees and nonfinancial support from PDX Pharma, personal fees, nonfinancial support, and other compensation from Signalchem (stock), personal fees and nonfinancial support from Symphogen, personal fees, nonfinancial support, and other compensation from Tarveda (stock), personal fees and nonfinancial support from Turbine and Zentalis, other compensation from Catena (stock), Genentech (clinical trials support), GSK (clinical trials support), grants from Adelson Medical Research Foundation, Breast Cancer Research Foundation, Komen Research Foundation, Ovarian Cancer Research Foundation, and Prospect Creek Foundation during the conduct of the study. N. Sahni reports grants from Breast Cancer Alliance, Ovarian Cancer Research Alliance, Alfred P. Sloan Foundation, and Cancer Prevention and Research Institute of Texas during the conduct of the study. S. Yi reports grants from Susan Komen Foundation and grants from NCI during the conduct of the study. No potential conflicts of interest were disclosed by the other authors. Publisher Copyright: © 2020 American Association for Cancer Research.

PY - 2020/11/1

Y1 - 2020/11/1

N2 - Alterations in immune-related pathways are common hallmarks of cancer. A comprehensive understanding of how cancer mutations rewire immune signaling networks and functional output across cancer types is instrumental to realize the full potential of immunotherapy. Here, we systematically interrogated somatic mutations involved in immune signaling that alter immune responses in patients with cancer. To do so, we developed a Network-based Integrative model to Prioritize Potential immune respondER genes (NIPPER). Identified mutations were enriched in essential protein domains and genes identified by NIPPER were associated with responsiveness to multiple immunotherapy modalities. These genes were used to devise an interactome network propagation framework integrated with drug-associated gene signatures to identify potential immunomodulatory drug candidates. Together, our systems-level analysis results help interpret the heterogeneous immune responses among patients and serve as a resource for future functional studies and targeted therapeutics.

AB - Alterations in immune-related pathways are common hallmarks of cancer. A comprehensive understanding of how cancer mutations rewire immune signaling networks and functional output across cancer types is instrumental to realize the full potential of immunotherapy. Here, we systematically interrogated somatic mutations involved in immune signaling that alter immune responses in patients with cancer. To do so, we developed a Network-based Integrative model to Prioritize Potential immune respondER genes (NIPPER). Identified mutations were enriched in essential protein domains and genes identified by NIPPER were associated with responsiveness to multiple immunotherapy modalities. These genes were used to devise an interactome network propagation framework integrated with drug-associated gene signatures to identify potential immunomodulatory drug candidates. Together, our systems-level analysis results help interpret the heterogeneous immune responses among patients and serve as a resource for future functional studies and targeted therapeutics.

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VL - 80

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JO - Cancer research

JF - Cancer research

IS - 21

ER -

Integrated genomic characterization of the human immunome in cancer

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