Literature DB >> 25401301

Spectrum of diverse genomic alterations define non-clear cell renal carcinoma subtypes.

Steffen Durinck1,2, Eric W Stawiski1,2, Andrea Pavía-Jiménez3,4,5, Zora Modrusan1, Payal Kapur3,6, Bijay S Jaiswal1, Na Zhang1, Vanina Toffessi-Tcheuyap3,4,5, Thong T Nguyen1, Kanika Bajaj Pahuja1, Ying-Jiun Chen1, Sadia Saleem3,4, Subhra Chaudhuri1, Sherry Heldens1, Marlena Jackson1, Samuel Peña-Llopis3,4,5, Joseph Guillory1, Karen Toy1, Connie Ha1, Corissa J Harris1, Eboni Holloman3,4,5, Haley M Hill3,4,5, Jeremy Stinson1, Celina Sanchez Rivers1, Vasantharajan Janakiraman1, Weiru Wang7, Lisa N Kinch3,8,9, Nick V Grishin3,8,9, Peter M Haverty2, Bernard Chow1, Julian S Gehring2, Jens Reeder2, Gregoire Pau2, Thomas D Wu2, Vitaly Margulis3,10, Yair Lotan3,10, Arthur Sagalowsky3,10, Ivan Pedrosa3,11,12, Frederic J de Sauvage13, James Brugarolas3,4,5, Somasekar Seshagiri1.   

Abstract

To further understand the molecular distinctions between kidney cancer subtypes, we analyzed exome, transcriptome and copy number alteration data from 167 primary human tumors that included renal oncocytomas and non-clear cell renal cell carcinomas (nccRCCs), consisting of papillary (pRCC), chromophobe (chRCC) and translocation (tRCC) subtypes. We identified ten significantly mutated genes in pRCC, including MET, NF2, SLC5A3, PNKD and CPQ. MET mutations occurred in 15% (10/65) of pRCC samples and included previously unreported recurrent activating mutations. In chRCC, we found TP53, PTEN, FAAH2, PDHB, PDXDC1 and ZNF765 to be significantly mutated. Gene expression analysis identified a five-gene set that enabled the molecular classification of chRCC, renal oncocytoma and pRCC. Using RNA sequencing, we identified previously unreported gene fusions, including ACTG1-MITF fusion. Ectopic expression of the ACTG1-MITF fusion led to cellular transformation and induced the expression of downstream target genes. Finally, we observed upregulation of the anti-apoptotic factor BIRC7 in MiTF-high RCC tumors, suggesting a potential therapeutic role for BIRC7 inhibitors.

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Year:  2014        PMID: 25401301      PMCID: PMC4489427          DOI: 10.1038/ng.3146

Source DB:  PubMed          Journal:  Nat Genet        ISSN: 1061-4036            Impact factor:   38.330


  97 in total

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2.  The somatic genomic landscape of chromophobe renal cell carcinoma.

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Journal:  Cancer Cell       Date:  2014-08-21       Impact factor: 31.743

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9.  Succinate dehydrogenase kidney cancer: an aggressive example of the Warburg effect in cancer.

Authors:  Christopher J Ricketts; Brian Shuch; Cathy D Vocke; Adam R Metwalli; Gennady Bratslavsky; Lindsay Middelton; Youfeng Yang; Ming-Hui Wei; Stephen E Pautler; James Peterson; Catherine A Stolle; Berton Zbar; Maria J Merino; Laura S Schmidt; Peter A Pinto; Ramaprasad Srinivasan; Karel Pacak; W Marston Linehan
Journal:  J Urol       Date:  2012-10-18       Impact factor: 7.450

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  135 in total

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2.  IGF2BP2 stabilized FBXL19-AS1 regulates the blood-tumour barrier permeability by negatively regulating ZNF765 by STAU1-mediated mRNA decay.

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4.  Genomic landscape and evolution of metastatic chromophobe renal cell carcinoma.

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Review 8.  Precision medicine from the renal cancer genome.

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Review 9.  The multiple paths towards MET receptor addiction in cancer.

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