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Literature DB >> 28614790

Genomic landscape and evolution of metastatic chromophobe renal cell carcinoma.

Jozefina Casuscelli^1,2, Nils Weinhold³, Gunes Gundem⁴, Lu Wang⁵, Emily C Zabor⁴, Esther Drill⁴, Patricia I Wang¹, Gouri J Nanjangud⁶, Almedina Redzematovic^1,7, Amrita M Nargund¹, Brandon J Manley⁸, Maria E Arcila⁵, Nicholas M Donin⁹, John C Cheville¹⁰, R Houston Thompson¹¹, Allan J Pantuck⁹, Paul Russo⁸, Emily H Cheng^1,5, William Lee³, Satish K Tickoo⁵, Irina Ostrovnaya⁴, Chad J Creighton¹², Elli Papaemmanuil⁴, Venkatraman E Seshan⁴, A Ari Hakimi⁸, James J Hsieh¹³.

Abstract

Chromophobe renal cell carcinoma (chRCC) typically shows ~7 chromosome losses (1, 2, 6, 10, 13, 17, and 21) and ~31 exonic somatic mutations, yet carries ~5%-10% metastatic incidence. Since extensive chromosomal losses can generate proteotoxic stress and compromise cellular proliferation, it is intriguing how chRCC, a tumor with extensive chromosome losses and a low number of somatic mutations, can develop lethal metastases. Genomic features distinguishing metastatic from nonmetastatic chRCC are unknown. An integrated approach, including whole-genome sequencing (WGS), targeted ultradeep cancer gene sequencing, and chromosome analyses (FACETS, OncoScan, and FISH), was performed on 79 chRCC patients including 38 metastatic (M-chRCC) cases. We demonstrate that TP53 mutations (58%), PTEN mutations (24%), and imbalanced chromosome duplication (ICD, duplication of ≥ 3 chromosomes) (25%) were enriched in M-chRCC. Reconstruction of the subclonal composition of paired primary-metastatic chRCC tumors supports the role of TP53, PTEN, and ICD in metastatic evolution. Finally, the presence of these 3 genomic features in primary tumors of both The Cancer Genome Atlas kidney chromophobe (KICH) (n = 64) and M-chRCC (n = 35) cohorts was associated with worse survival. In summary, our study provides genomic insights into the metastatic progression of chRCC and identifies TP53 mutations, PTEN mutations, and ICD as high-risk features.

Entities: Disease Gene Species

Keywords: Genetics; Oncology

Year: 2017 PMID： 28614790 PMCID： PMC5470887 DOI： 10.1172/jci.insight.92688

Source DB: PubMed Journal: JCI Insight ISSN： 2379-3708

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