Multilevel Genomics-Based Taxonomy of Renal Cell Carcinoma

Fengju Chen; Yiqun Zhang; Yasin Şenbabaoğlu; Giovanni Ciriello; Lixing Yang; Ed Reznik; Brian Shuch; Goran Micevic; Guillermo de Velasco; Eve Shinbrot; Michael S. Noble; Yiling Lu; Kyle R. Covington; Xi Liu; Jennifer Drummond; Donna M. Muzny; Hyojin Kang; Junehawk Lee; Pheroze Tamboli; Victor E. Reuter; Carl Simon Shelley; Benny Abraham Kaipparettu; Donald P. Bottaro; Andrew K. Godwin; Richard A. Gibbs; Gad Getz; Raju Kucherlapati; Peter J. Park; Chris Sander; Elizabeth P. Henske; Jane H. Zhou; David J. Kwiatkowski; Thai H. Ho; Toni K. Choueiri; James J. Hsieh; Rehan Akbani; Gordon B. Mills; A. Ari Hakimi; David A. Wheeler; Chad J. Creighton

doi:10.1016/j.celrep.2016.02.024

Multilevel Genomics-Based Taxonomy of Renal Cell Carcinoma

Fengju Chen(Baylor College of Medicine), Yiqun Zhang(Baylor College of Medicine), Yasin Şenbabaoğlu(Memorial Sloan Kettering Cancer Center), Giovanni Ciriello(University of Lausanne), Lixing Yang(Harvard University), Ed Reznik(Memorial Sloan Kettering Cancer Center), Brian Shuch(Yale University), Goran Micevic(Yale University), Guillermo de Velasco(Dana-Farber Cancer Institute), Eve Shinbrot(Baylor College of Medicine), Michael S. Noble(Broad Institute), Yiling Lu(The University of Texas MD Anderson Cancer Center), Kyle R. Covington(Baylor College of Medicine), Xi Liu(Baylor College of Medicine), Jennifer Drummond(Baylor College of Medicine), Donna M. Muzny(Baylor College of Medicine), Hyojin Kang(Korea Advanced Institute of Science and Technology), Junehawk Lee(Korea Advanced Institute of Science and Technology), Pheroze Tamboli(The University of Texas MD Anderson Cancer Center), Victor E. Reuter(Memorial Sloan Kettering Cancer Center), Carl Simon Shelley(University of Wisconsin–Madison), Benny Abraham Kaipparettu(Baylor College of Medicine), Donald P. Bottaro(National Cancer Institute), Andrew K. Godwin(University of Kansas Medical Center), Richard A. Gibbs(Baylor College of Medicine), Gad Getz(Broad Institute), Raju Kucherlapati(Brigham and Women's Hospital), Peter J. Park(Harvard University), Chris Sander(Memorial Sloan Kettering Cancer Center), Elizabeth P. Henske(Broad Institute), Jane H. Zhou(Tufts University), David J. Kwiatkowski(Broad Institute), Thai H. Ho(Mayo Clinic in Arizona), Toni K. Choueiri(Dana-Farber Cancer Institute), James J. Hsieh(Memorial Sloan Kettering Cancer Center), Rehan Akbani(The University of Texas MD Anderson Cancer Center), Gordon B. Mills(The University of Texas MD Anderson Cancer Center), A. Ari Hakimi(Memorial Sloan Kettering Cancer Center), David A. Wheeler(Baylor College of Medicine), Chad J. Creighton(The University of Texas MD Anderson Cancer Center)

Cell Reports

March 1, 2016

10.1016/j.celrep.2016.02.024

Cited by 380Open Access

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Abstract

On the basis of multidimensional and comprehensive molecular characterization (including DNA methalylation and copy number, RNA, and protein expression), we classified 894 renal cell carcinomas (RCCs) of various histologic types into nine major genomic subtypes. Site of origin within the nephron was one major determinant in the classification, reflecting differences among clear cell, chromophobe, and papillary RCC. Widespread molecular changes associated with TFE3 gene fusion or chromatin modifier genes were present within a specific subtype and spanned multiple subtypes. Differences in patient survival and in alteration of specific pathways (including hypoxia, metabolism, MAP kinase, NRF2-ARE, Hippo, immune checkpoint, and PI3K/AKT/mTOR) could further distinguish the subtypes. Immune checkpoint markers and molecular signatures of T cell infiltrates were both highest in the subtype associated with aggressive clear cell RCC. Differences between the genomic subtypes suggest that therapeutic strategies could be tailored to each RCC disease subset.

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