| Literature DB >> 27699219 |
Dijana Djureinovic1, Björn M Hallström2, Masafumi Horie3, Johanna Sofia Margareta Mattsson1, Linnea La Fleur1, Linn Fagerberg2, Hans Brunnström4, Cecilia Lindskog1, Katrin Madjar5, Jörg Rahnenführer5, Simon Ekman6, Elisabeth Ståhle7, Hirsh Koyi8, Eva Brandén8, Karolina Edlund9, Jan G Hengstler9, Mats Lambe10, Akira Saito3, Johan Botling1, Fredrik Pontén1, Mathias Uhlén2, Patrick Micke1.
Abstract
Cancer testis antigens (CTAs) are of clinical interest as biomarkers and present valuable targets for immunotherapy. To comprehensively characterize the CTA landscape of non-small-cell lung cancer (NSCLC), we compared RNAseq data from 199 NSCLC tissues to the normal transcriptome of 142 samples from 32 different normal organs. Of 232 CTAs currently annotated in the Caner Testis Database (CTdatabase), 96 were confirmed in NSCLC. To obtain an unbiased CTA profile of NSCLC, we applied stringent criteria on our RNAseq data set and defined 90 genes as CTAs, of which 55 genes were not annotated in the CTdatabase, thus representing potential new CTAs. Cluster analysis revealed that CTA expression is histology dependent and concurrent expression is common. IHC confirmed tissue-specific protein expression of selected new CTAs (TKTL1, TGIF2LX, VCX, and CXORF67). Furthermore, methylation was identified as a regulatory mechanism of CTA expression based on independent data from The Cancer Genome Atlas. The proposed prognostic impact of CTAs in lung cancer was not confirmed, neither in our RNAseq cohort nor in an independent meta-analysis of 1,117 NSCLC cases. In summary, we defined a set of 90 reliable CTAs, including information on protein expression, methylation, and survival association. The detailed RNAseq catalog can guide biomarker studies and efforts to identify targets for immunotherapeutic strategies.Entities:
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Year: 2016 PMID: 27699219 PMCID: PMC5033889 DOI: 10.1172/jci.insight.86837
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708