Epigenomic charting and functional annotation of risk loci in renal cell carcinoma

Author:

Nassar Amin H.ORCID,Abou Alaiwi Sarah,Baca Sylvan C.,Adib Elio,Corona Rosario I.ORCID,Seo Ji-Heui,Fonseca Marcos A. S.,Spisak SandorORCID,El Zarif Talal,Tisza Viktoria,Braun David A.ORCID,Du HengORCID,He Monica,Flaifel Abdallah,Alchoueiry MichelORCID,Denize Thomas,Matar Sayed G.,Acosta Andres,Shukla SachetORCID,Hou Yue,Steinharter John,Bouchard Gabrielle,Berchuck Jacob E.ORCID,O’Connor Edward,Bell ConnorORCID,Nuzzo Pier VitaleORCID,Mary Lee Gwo-Shu,Signoretti Sabina,Hirsch Michelle S.ORCID,Pomerantz Mark,Henske ElizabethORCID,Gusev AlexanderORCID,Lawrenson KateORCID,Choueiri Toni K.ORCID,Kwiatkowski David J.ORCID,Freedman Matthew L.ORCID

Abstract

AbstractWhile the mutational and transcriptional landscapes of renal cell carcinoma (RCC) are well-known, the epigenome is poorly understood. We characterize the epigenome of clear cell (ccRCC), papillary (pRCC), and chromophobe RCC (chRCC) by using ChIP-seq, ATAC-Seq, RNA-seq, and SNP arrays. We integrate 153 individual data sets from 42 patients and nominate 50 histology-specific master transcription factors (MTF) to define RCC histologic subtypes, including EPAS1 and ETS-1 in ccRCC, HNF1B in pRCC, and FOXI1 in chRCC. We confirm histology-specific MTFs via immunohistochemistry including a ccRCC-specific TF, BHLHE41. FOXI1 overexpression with knock-down of EPAS1 in the 786-O ccRCC cell line induces transcriptional upregulation of chRCC-specific genes, TFCP2L1, ATP6V0D2, KIT, and INSRR, implicating FOXI1 as a MTF for chRCC. Integrating RCC GWAS risk SNPs with H3K27ac ChIP-seq and ATAC-seq data reveals that risk-variants are significantly enriched in allelically-imbalanced peaks. This epigenomic atlas in primary human samples provides a resource for future investigation.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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