Exome sequencing identifies frequent mutation of the SWI/SNF complex gene PBRM1 in renal carcinoma

Ignacio Varela; Patrick Tarpey; Keiran Raine; Dachuan Huang; Choon Kiat Ong; Philip Stephens; Helen Davies; David Jones; Meng Lin; Jon W. Teague; Graham R. Bignell; Adam P. Butler; Juok Cho; Gillian L. Dalgliesh; Danushka Galappaththige; Chris Greenman; Claire Hardy; Mingming Jia; Calli Latimer; King Wai Lau; John L. Marshall; Stuart McLaren; Andrew Menzies; Laura Mudie; Lucy Stebbings; David A. Largaespada; Lodewyk F.A. Wessels; Stephane Richard; Richard J. Kahnoski; John Anema; David A. Tuveson; Pedro A. Pérez–Mancera; Ville Mustonen; Andrej Fischer; David J. Adams; Alistair G. Rust; Waraporn Chan-on; Chutima Subimerb; Karl Dykema; Kyle Furge; Peter J. Campbell; Bin Tean Teh; Michael R. Stratton; P. Andrew Futreal

doi:10.1038/nature09639

Exome sequencing identifies frequent mutation of the SWI/SNF complex gene PBRM1 in renal carcinoma

Ignacio Varela(Wellcome Sanger Institute), Patrick Tarpey(Wellcome Sanger Institute), Keiran Raine(Wellcome Sanger Institute), Dachuan Huang(National Cancer Centre Japan), Choon Kiat Ong(National Cancer Centre Japan), Philip Stephens(Wellcome Sanger Institute), Helen Davies(Wellcome Sanger Institute), David Jones(Wellcome Sanger Institute), Meng Lin(Wellcome Sanger Institute), Jon W. Teague(Wellcome Sanger Institute), Graham R. Bignell(Wellcome Sanger Institute), Adam P. Butler(Wellcome Sanger Institute), Juok Cho(Wellcome Sanger Institute), Gillian L. Dalgliesh(Wellcome Sanger Institute), Danushka Galappaththige(Wellcome Sanger Institute), Chris Greenman(Wellcome Sanger Institute), Claire Hardy(Wellcome Sanger Institute), Mingming Jia(Wellcome Sanger Institute), Calli Latimer(Wellcome Sanger Institute), King Wai Lau(Wellcome Sanger Institute), John L. Marshall(Wellcome Sanger Institute), Stuart McLaren(Wellcome Sanger Institute), Andrew Menzies(Wellcome Sanger Institute), Laura Mudie(Wellcome Sanger Institute), Lucy Stebbings(Wellcome Sanger Institute), David A. Largaespada(University of Minnesota), Lodewyk F.A. Wessels(The Netherlands Cancer Institute), Stephane Richard(Université Paris-Sud), Richard J. Kahnoski(Spectrum Health), John Anema(Spectrum Health), David A. Tuveson(Cancer Research UK), Pedro A. Pérez–Mancera(Cancer Research UK), Ville Mustonen(Wellcome Sanger Institute), Andrej Fischer(University of Cologne), David J. Adams(Wellcome Sanger Institute), Alistair G. Rust(Wellcome Sanger Institute), Waraporn Chan-on(National Cancer Centre Japan), Chutima Subimerb(National Cancer Centre Japan), Karl Dykema(Van Andel Institute), Kyle Furge(Van Andel Institute), Peter J. Campbell(Wellcome Sanger Institute), Bin Tean Teh(Van Andel Institute), Michael R. Stratton(Institute of Cancer Research), P. Andrew Futreal(Wellcome Sanger Institute)

Nature

January 19, 2011

10.1038/nature09639

Cited by 1,284Open Access

Full Text

Abstract

Using large-scale exome sequencing, Andrew Futreal and colleagues have identified a second frequently mutated gene (after VHL) in clear cell renal cell carcinomas, the most frequent type of kidney cancer. PBRM1, a member of the SWI/SNF complex involved in transcriptional regulation, is mutated in about 40% of cases and is shown to function as a tumour suppressor gene. PBRM1 was independently found as a putative cancer gene involved in pancreatic cancer in a mouse transposon screen. These results — together with the fact that other components of the same complex are known cancer genes — unambiguously identify PBRM1 as a major cancer gene. Using large-scale exome sequencing, this study identifies a second (after VHL) frequently mutated gene in clear cell renal cell carcinomas, the most frequent type of kidney cancer. PBRM1, a member of the SWI/SNF complex involved in transcriptional regulation, is mutated in about 40% of cases and shown to function as tumour suppressor gene. PBRM1 was independently found as a putative cancer gene involved in pancreatic cancer in a mouse transposon screen. The genetics of renal cancer is dominated by inactivation of the VHL tumour suppressor gene in clear cell carcinoma (ccRCC), the commonest histological subtype. A recent large-scale screen of ∼3,500 genes by PCR-based exon re-sequencing identified several new cancer genes in ccRCC including UTX (also known as KDM6A)1, JARID1C (also known as KDM5C) and SETD2 (ref. 2). These genes encode enzymes that demethylate (UTX, JARID1C) or methylate (SETD2) key lysine residues of histone H3. Modification of the methylation state of these lysine residues of histone H3 regulates chromatin structure and is implicated in transcriptional control3. However, together these mutations are present in fewer than 15% of ccRCC, suggesting the existence of additional, currently unidentified cancer genes. Here, we have sequenced the protein coding exome in a series of primary ccRCC and report the identification of the SWI/SNF chromatin remodelling complex gene PBRM1 (ref. 4) as a second major ccRCC cancer gene, with truncating mutations in 41% (92/227) of cases. These data further elucidate the somatic genetic architecture of ccRCC and emphasize the marked contribution of aberrant chromatin biology.

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Exome sequencing identifies frequent mutation of the SWI/SNF complex gene PBRM1 in renal carcinoma

Abstract

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