Pan-cancer proteogenomics connects oncogenic drivers to functional states

Clinical Proteomic Tumor Analysis Consortium

doi:10.1016/j.cell.2023.07.014

Pan-cancer proteogenomics connects oncogenic drivers to functional states

Clinical Proteomic Tumor Analysis Consortium

Washington University St. Louis
Josep Carreras Leukaemia Research Institute
Barcelona Supercomputing Center (BSC)
Dana-Farber Cancer Institute
Harvard University
Brigham Young University
Cornell University
University of Miami
Broad Institute
MGH Cancer Center and Department of Pathology
New York University
Icahn School of Medicine at Mount Sinai
University of Michigan, Ann Arbor
University of Sannio
National Institutes of Health
University of Texas MD Anderson Cancer Center

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

77 Scopus citations

Abstract

Cancer driver events refer to key genetic aberrations that drive oncogenesis; however, their exact molecular mechanisms remain insufficiently understood. Here, our multi-omics pan-cancer analysis uncovers insights into the impacts of cancer drivers by identifying their significant cis-effects and distal trans-effects quantified at the RNA, protein, and phosphoprotein levels. Salient observations include the association of point mutations and copy-number alterations with the rewiring of protein interaction networks, and notably, most cancer genes converge toward similar molecular states denoted by sequence-based kinase activity profiles. A correlation between predicted neoantigen burden and measured T cell infiltration suggests potential vulnerabilities for immunotherapies. Patterns of cancer hallmarks vary by polygenic protein abundance ranging from uniform to heterogeneous. Overall, our work demonstrates the value of comprehensive proteogenomics in understanding the functional states of oncogenic drivers and their links to cancer development, surpassing the limitations of studying individual cancer types.

Original language	English
Pages (from-to)	3921-3944.e25
Journal	Cell
Volume	186
Issue number	18
DOIs	https://doi.org/10.1016/j.cell.2023.07.014
State	Published - 31 Aug 2023
Externally published	Yes

Bibliographical note

Publisher Copyright:
© 2023 The Authors

UN SDGs

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

SDG 3 Good Health and Well-being

Keywords

CPTAC
cancer hallmark
oncogenic driver
pan-cancer
phosphoproteomics
protein complex
proteogenomics
proteomics
therapeutic target

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10.1016/j.cell.2023.07.014

Cite this

@article{695f43b2281c4c949a45332e6275c694,

title = "Pan-cancer proteogenomics connects oncogenic drivers to functional states",

abstract = "Cancer driver events refer to key genetic aberrations that drive oncogenesis; however, their exact molecular mechanisms remain insufficiently understood. Here, our multi-omics pan-cancer analysis uncovers insights into the impacts of cancer drivers by identifying their significant cis-effects and distal trans-effects quantified at the RNA, protein, and phosphoprotein levels. Salient observations include the association of point mutations and copy-number alterations with the rewiring of protein interaction networks, and notably, most cancer genes converge toward similar molecular states denoted by sequence-based kinase activity profiles. A correlation between predicted neoantigen burden and measured T cell infiltration suggests potential vulnerabilities for immunotherapies. Patterns of cancer hallmarks vary by polygenic protein abundance ranging from uniform to heterogeneous. Overall, our work demonstrates the value of comprehensive proteogenomics in understanding the functional states of oncogenic drivers and their links to cancer development, surpassing the limitations of studying individual cancer types.",

keywords = "CPTAC, cancer hallmark, oncogenic driver, pan-cancer, phosphoproteomics, protein complex, proteogenomics, proteomics, therapeutic target",

author = "\{Clinical Proteomic Tumor Analysis Consortium\} and Yize Li and Eduard Porta-Pardo and Collin Tokheim and Bailey, \{Matthew H.\} and Yaron, \{Tomer M.\} and Vasileios Stathias and Yifat Geffen and Imbach, \{Kathleen J.\} and Song Cao and Shankara Anand and Yo Akiyama and Wenke Liu and Wyczalkowski, \{Matthew A.\} and Yizhe Song and Storrs, \{Erik P.\} and Wendl, \{Michael C.\} and Wubing Zhang and Mustafa Sibai and Victoria Ruiz-Serra and Liang, \{Wen Wei\} and Terekhanova, \{Nadezhda V.\} and Rodrigues, \{Fernanda Martins\} and Clauser, \{Karl R.\} and Heiman, \{David I.\} and Qing Zhang and Francois Aguet and Calinawan, \{Anna P.\} and Dhanasekaran, \{Saravana M.\} and Chet Birger and Shankha Satpathy and Zhou, \{Daniel Cui\} and Wang, \{Liang Bo\} and Jessika Baral and Johnson, \{Jared L.\} and Huntsman, \{Emily M.\} and Pietro Pugliese and Antonio Colaprico and Antonio Iavarone and Chheda, \{Milan G.\} and Ricketts, \{Christopher J.\} and David Feny{\"o} and Payne, \{Samuel H.\} and Henry Rodriguez and Robles, \{Ana I.\} and Gillette, \{Michael A.\} and Chandan Kumar-Sinha and Lazar, \{Alexander J.\} and Cantley, \{Lewis C.\} and Gad Getz and Li Ding",

note = "Publisher Copyright: {\textcopyright} 2023 The Authors",

year = "2023",

month = aug,

day = "31",

doi = "10.1016/j.cell.2023.07.014",

language = "אנגלית",

volume = "186",

pages = "3921--3944.e25",

journal = "Cell",

issn = "0092-8674",

publisher = "Elsevier B.V.",

number = "18",

}

TY - JOUR

T1 - Pan-cancer proteogenomics connects oncogenic drivers to functional states

AU - Clinical Proteomic Tumor Analysis Consortium

AU - Li, Yize

AU - Porta-Pardo, Eduard

AU - Tokheim, Collin

AU - Bailey, Matthew H.

AU - Yaron, Tomer M.

AU - Stathias, Vasileios

AU - Geffen, Yifat

AU - Imbach, Kathleen J.

AU - Cao, Song

AU - Anand, Shankara

AU - Akiyama, Yo

AU - Liu, Wenke

AU - Wyczalkowski, Matthew A.

AU - Song, Yizhe

AU - Storrs, Erik P.

AU - Wendl, Michael C.

AU - Zhang, Wubing

AU - Sibai, Mustafa

AU - Ruiz-Serra, Victoria

AU - Liang, Wen Wei

AU - Terekhanova, Nadezhda V.

AU - Rodrigues, Fernanda Martins

AU - Clauser, Karl R.

AU - Heiman, David I.

AU - Zhang, Qing

AU - Aguet, Francois

AU - Calinawan, Anna P.

AU - Dhanasekaran, Saravana M.

AU - Birger, Chet

AU - Satpathy, Shankha

AU - Zhou, Daniel Cui

AU - Wang, Liang Bo

AU - Baral, Jessika

AU - Johnson, Jared L.

AU - Huntsman, Emily M.

AU - Pugliese, Pietro

AU - Colaprico, Antonio

AU - Iavarone, Antonio

AU - Chheda, Milan G.

AU - Ricketts, Christopher J.

AU - Fenyö, David

AU - Payne, Samuel H.

AU - Rodriguez, Henry

AU - Robles, Ana I.

AU - Gillette, Michael A.

AU - Kumar-Sinha, Chandan

AU - Lazar, Alexander J.

AU - Cantley, Lewis C.

AU - Getz, Gad

AU - Ding, Li

PY - 2023/8/31

Y1 - 2023/8/31

N2 - Cancer driver events refer to key genetic aberrations that drive oncogenesis; however, their exact molecular mechanisms remain insufficiently understood. Here, our multi-omics pan-cancer analysis uncovers insights into the impacts of cancer drivers by identifying their significant cis-effects and distal trans-effects quantified at the RNA, protein, and phosphoprotein levels. Salient observations include the association of point mutations and copy-number alterations with the rewiring of protein interaction networks, and notably, most cancer genes converge toward similar molecular states denoted by sequence-based kinase activity profiles. A correlation between predicted neoantigen burden and measured T cell infiltration suggests potential vulnerabilities for immunotherapies. Patterns of cancer hallmarks vary by polygenic protein abundance ranging from uniform to heterogeneous. Overall, our work demonstrates the value of comprehensive proteogenomics in understanding the functional states of oncogenic drivers and their links to cancer development, surpassing the limitations of studying individual cancer types.

AB - Cancer driver events refer to key genetic aberrations that drive oncogenesis; however, their exact molecular mechanisms remain insufficiently understood. Here, our multi-omics pan-cancer analysis uncovers insights into the impacts of cancer drivers by identifying their significant cis-effects and distal trans-effects quantified at the RNA, protein, and phosphoprotein levels. Salient observations include the association of point mutations and copy-number alterations with the rewiring of protein interaction networks, and notably, most cancer genes converge toward similar molecular states denoted by sequence-based kinase activity profiles. A correlation between predicted neoantigen burden and measured T cell infiltration suggests potential vulnerabilities for immunotherapies. Patterns of cancer hallmarks vary by polygenic protein abundance ranging from uniform to heterogeneous. Overall, our work demonstrates the value of comprehensive proteogenomics in understanding the functional states of oncogenic drivers and their links to cancer development, surpassing the limitations of studying individual cancer types.

KW - CPTAC

KW - cancer hallmark

KW - oncogenic driver

KW - pan-cancer

KW - phosphoproteomics

KW - protein complex

KW - proteogenomics

KW - proteomics

KW - therapeutic target

UR - https://www.scopus.com/pages/publications/85169624163

U2 - 10.1016/j.cell.2023.07.014

DO - 10.1016/j.cell.2023.07.014

M3 - ???researchoutput.researchoutputtypes.contributiontojournal.article???

C2 - 37582357

AN - SCOPUS:85169624163

SN - 0092-8674

VL - 186

SP - 3921-3944.e25

JO - Cell

JF - Cell

IS - 18

ER -

Pan-cancer proteogenomics connects oncogenic drivers to functional states

Abstract

Bibliographical note

UN SDGs

Keywords

Access to Document

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