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Integrated Proteogenomic Characterization of Clear Cell Renal Cell Carcinoma

Authors :
David J. Clark
Jianbo Pan
Gerald W. Hart
Katherine A. Hoadley
Negin Vatanian
Shuang Cai
Yige Wu
Felipe da Veiga Leprevost
A. Ari Hakimi
Sanford P. Markey
Thomas F. Westbrook
Maciej Wiznerowicz
Nathan Edwards
Alla Y. Karpova
Sohini Sengupta
Marcin Cieslik
Samuel H. Payne
Xi Steven Chen
Guo Ci Teo
Jin Chen
Boris Reva
Corbin D. Jones
Michael J. Birrer
Ying Wang
Kelly V. Ruggles
Doug W. Chan
John McGee
Marcin J. Domagalski
Song Cao
Linda Hannick
Christopher R. Kinsinger
David I. Heiman
Jennifer M. Eschbacher
Munziba Khan
Jason E. McDermott
Dmitry M. Avtonomov
Sue Hilsenbeck
Qing Kay Li
Jiayi Ji
Emek Demir
Rebecca I. Montgomery
Qingsong Gao
Beom-Jun Kim
Xiaoyu Song
Karl R. Clauser
Christian P. Pavlovich
Richard D. Smith
Maureen Dyer
Jeffrey W. Tyner
Amy M. Perou
Yuping Zhang
Dana R. Valley
George D. Wilson
Shiyong Ma
Minghui Ao
Jiang Qian
Umut Ozbek
Melissa Borucki
Zhi Li
Michael Schnaubelt
Chen Huang
Piotr A. Mieczkowski
Francesca Petralia
Abdul Samad Hashimi
Hui Yin Chang
Liang-Bo Wang
Matthew E. Monroe
Peter B. McGarvey
Tao Liu
Karen A. Ketchum
Hui Zhang
Bing Zhang
D. R. Mani
Houston Culpepper
Hua Zhou
Saravana M. Dhanasekaran
Paul D. Piehowski
Zhidong Tu
Brian J. Druker
Ki Sung Um
Zhiao Shi
Uma Borate
Uma Velvulou
Michael Ittmann
Weiping Ma
Steven M. Foltz
Heng Zhu
Stacey Gabriel
Hongwei Liu
Ramani B. Kothadia
Lin Chen
Ewa P. Malc
Marina A. Gritsenko
Jun Zhu
David Chesla
Lori J. Sokoll
Stephen E. Stein
Andrzej Antczak
Matthew L. Anderson
Alyssa Charamut
Pamela Grady
Michael T. Lewis
Shannon Richey
Tanya Krubit
Alexander R. Pico
Kyung-Cho Cho
Daniel C. Rohrer
Francesmary Modugno
Stephanie De Young
Li Ding
Michael Smith
Mathangi Thiagarajan
Alexey I. Nesvizhskii
Shrabanti Chowdhury
Noam D. Beckmann
Kimberly R. Holloway
Ratna R. Thangudu
Sherri R. Davies
Tung-Shing M. Lih
Nicole Tignor
Anna Calinawan
Meghan C. Burke
Karna Robinson
Chet Birger
Shalin Patel
Antonio Colaprico
Sarah Keegan
Daniel J. Geiszler
Scott D. Jewell
William Bocik
Snehal Patil
Pei Wang
MacIntosh Cornwell
Emily Kawaler
Seungyeul Yoo
Jasmine Huang
Vladislav A. Petyuk
Ross Bremner
Donghui Tan
Stefani N. Thomas
Emily S. Boja
Anna Malovannaya
Xi Chen
Wenke Liu
Eric E. Schadt
Shankha Satpathy
Nancy Roche
Rajiv Dhir
Cristina E. Tognon
Michelle Chaikin
Gabriel Bromiński
Daniel C. Zhou
Yifat Geffen
Tara Skelly
Jacob J. Day
Sunantha Sethuraman
Sonya Carter
Zhen Zhang
Selim Kalayci
Michael Vernon
Zeynep H. Gümüş
Kai Li
Barbara Hindenach
Matthew J. Ellis
Meenakshi Anurag
David C. Wheeler
Sailaja Mareedu
Andy T. Kong
Arul M. Chinnaiyan
Robert Zelt
Annette Marrero-Oliveras
Henry Rodriguez
James Suh
Anupriya Agarwal
David Fenyö
Galen Hostetter
Liqun Qi
Matthew A. Wyczalkowski
W. Marston Linehan
Tara Hiltke
Feng Chen
Lijun Chen
Jan Lubinski
Chelsea J. Newton
Steven A. Carr
Tatiana Omelchenko
Gilbert S. Omenn
Karsten Krug
Ana I. Robles
Azra Krek
Runyu Hong
Milan G. Chheda
Yize Li
Yan Shi
Lili Blumenberg
Ruiyang Liu
Karin D. Rodland
Hua Sun
Kim Elburn
Jeffrey R. Whiteaker
Christopher J. Ricketts
Gaddy Getz
Daniel W. Chan
Bo Wen
Robert Edwards
Patricia Castro
Yingwei Hu
Pushpa Hariharan
Simina M. Boca
Darlene Tansil
Phillip M. Pierorazio
Yosef E. Maruvka
Sandra Cottingham
James J. Hsieh
Amanda G. Paulovich
Barbara Pruetz
Michael A. Gillette
Yihao Lu
Dmitry Rykunov
Mehdi Mesri
Marc M. Loriaux
Reyka G Jayasinghe
Suhas Vasaikar
Source :
Cell
Publication Year :
2020
Publisher :
Elsevier BV, 2020.

Abstract

SUMMARY To elucidate the deregulated functional modules that drive clear cell renal cell carcinoma (ccRCC), we performed comprehensive genomic, epigenomic, transcriptomic, proteomic, and phosphoproteomic characterization of treatment-naive ccRCC and paired normal adjacent tissue samples. Genomic analyses identified a distinct molecular subgroup associated with genomic instability. Integration of proteogenomic measurements uniquely identified protein dysregulation of cellular mechanisms impacted by genomic alterations, including oxidative phosphorylation-related metabolism, protein translation processes, and phospho-signaling modules. To assess the degree of immune infiltration in individual tumors, we identified microenvironment cell signatures that delineated four immune-based ccRCC subtypes characterized by distinct cellular pathways. This study reports a large-scale proteogenomic analysis of ccRCC to discern the functional impact of genomic alterations and provides evidence for rational treatment selection stemming from ccRCC pathobiology.<br />Graphical Abstract<br />In Brief Comprehensive proteogenomic characterization in 103 treatment-naive clear cell renal cell carcinoma patient samples highlights tumor-specific alterations at the proteomic level that are unrevealed by transcriptomic profiling and proposes a revised subtyping scheme based on integrated omics analysis.

Details

ISSN :
00928674
Volume :
180
Database :
OpenAIRE
Journal :
Cell
Accession number :
edsair.doi.dedup.....a7b0db3ed2c470e7d44e149915509d50