Elsevier

Neoplasia

Volume 15, Issue 11, November 2013, Pages 1231-1240
Neoplasia

Identification of Molecular Tumor Markers in Renal Cell Carcinomas with TFE3 Protein Expression by RNA Sequencing1,2

https://doi.org/10.1593/neo.131544Get rights and content
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open access

Abstract

TFE3 translocation renal cell carcinoma (tRCC) is defined by chromosomal translocations involving the TFE3 transcription factor at chromosome Xp11.2. Genetically proven TFE3 tRCCs have a broad histologic spectrum with overlapping features to other renal tumor subtypes. In this study,we aimed for characterizing RCC with TFE3 protein expression. Using next-generation whole transcriptome sequencing (RNA-Seq) as a discovery tool, we analyzed fusion transcripts, gene expression profile, and somatic mutations in frozen tissue of one TFE3 tRCC. By applying a computational analysis developed to call chimeric RNA molecules from paired-end RNA-Seq data, we confirmed the known TFE3 translocation. Its fusion partner SFPQ has already been described as fusion partner in tRCCs. In addition, an RNAread-through chimera between TMED6 and COG8 as well as MET and KDR (VEGFR2) point mutations were identified. An EGFR mutation, but no chromosomal rearrangements, was identified in a control group of five clear cell RCCs (ccRCCs). The TFE3 tRCC could be clearly distinguished from the ccRCCs by RNA-Seq gene expression measurements using a previously reported tRCC gene signature. In validation experiments using reverse transcription-PCR, TMED6-COG8 chimera expression was significantly higher in nine TFE3 translocated and six TFE3-expressing/non-translocated RCCs than in 24 ccRCCs (P<.001) and 22 papillaryRCCs (P<.05-.07). Immunohistochemical analysis of selected genes from the tRCC gene signature showed significantly higher eukaryotic translation elongation factor 1 alpha 2 (EEF1A2) and Contactin 3 (CNTN3) expression in 16 TFE3 translocated and six TFE3-expressing/non-translocated RCCs than in over 200 ccRCCs (P < .0001, both).

Abbreviations

AA
amino acid
ccRCC
clear cell renal cell carcinoma
CDS
coding DNA sequence
FISH
fluorescence in situ hybridization
IHC
immunohistochemistry
PE,
paired-end
RCC
renal cell carcinoma
RNA-Seq
next-generation whole transcriptome sequencing
RT-PCR
reverse transcription-polymerase chain reaction
TMA
tissue microarray
tRCC
translocation renal cell carcinoma
VHL
von Hippel-Lindau

Cited by (0)

1

This work was funded by the Swiss National Science Foundation (grant 135792; H.M.) and a Matching Fund of the University Hospital Zurich (D.P.). M.A.R. serves as a consultant to Gen-Probe, Inc and Ventana Medical Systems, Inc. Gen-Probe and Ventana have not played a role in the design and conduct of the study; in the collection, analysis, or interpretation of the data; or in the preparation, review, or approval of the manuscript. The other authors disclose no potential conflicts of interest.

2

This article refers to supplementary materials, which are designated by Tables W1 to W4 and are available online at www.neoplasia.com