Frequent copy number gains of SLC2A3 and ETV1 in testicular embryonal carcinomas

Author:

Hoff Andreas M1,Kraggerud Sigrid M1,Alagaratnam Sharmini1,Berg Kaja C G1,Johannessen Bjarne1,Høland Maren12,Nilsen Gro3,Lingjærde Ole C3,Andrews Peter W4,Lothe Ragnhild A12,Skotheim Rolf I13

Affiliation:

1. 1Department of Molecular Oncology, Institute for Cancer Research, The Norwegian Radium Hospital, Oslo University Hospital, Oslo, Norway

2. 2Institute for Clinical Medicine, Faculty of Medicine, University of Oslo, Oslo, Norway

3. 3Department of Informatics, Faculty of Mathematics and Natural Sciences, University of Oslo, Oslo, Norway

4. 4The Centre for Stem Cell Biology, Department of Biomedical Science, The University of Sheffield, Sheffield, UK

Abstract

Testicular germ cell tumours (TGCTs) appear as different histological subtypes or mixtures of these. They show similar, multiple DNA copy number changes, where gain of 12p is pathognomonic. However, few high-resolution analyses have been performed and focal DNA copy number changes with corresponding candidate target genes remain poorly described for individual subtypes. We present the first high-resolution DNA copy number aberration (CNA) analysis on the subtype embryonal carcinomas (ECs), including 13 primary ECs and 5 EC cell lines. We identified recurrent gains and losses and allele-specific CNAs. Within these regions, we nominate 30 genes that may be of interest to the EC subtype. By in silico analysis of data from 150 TGCTs from The Cancer Genome Atlas (TCGA), we further investigated CNAs, RNA expression, somatic mutations and fusion transcripts of these genes. Among primary ECs, ploidy ranged between 2.3 and 5.0, and the most common aberrations were DNA copy number gains at chromosome (arm) 7, 8, 12p, and 17, losses at 4, 10, 11, and 18, replicating known TGCT genome characteristics. Gain of whole or parts of 12p was found in all samples, including a highly amplified 100 kbp segment at 12p13.31, containing SLC2A3. Gain at 7p21, encompassing ETV1, was the second most frequent aberration. In conclusion, we present novel CNAs and the genes located within these regions, where the copy number gain of SLC2A3 and ETV1 are of interest, and which copy number levels also correlate with expression in TGCTs.

Publisher

Bioscientifica

Subject

Cancer Research,Endocrinology,Oncology,Endocrinology, Diabetes and Metabolism

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