Fusion sequencing via terminator-assisted synthesis (FTAS-seq) identifies TMPRSS2 fusion partners in prostate cancer

被引:3
作者
Drazdauskiene, Ugne [1 ]
Kapustina, Zana [1 ,4 ]
Medziune, Justina [1 ]
Dubovskaja, Varvara [1 ]
Sabaliauskaite, Rasa [2 ]
Jarmalaite, Sonata [2 ,3 ]
Lubys, Arvydas [1 ,4 ]
机构
[1] Thermo Fisher Sci Balt, Vilnius, Lithuania
[2] NCI, Vilnius, Lithuania
[3] Vilnius Univ, Inst Biosci, Life Sci Ctr, Vilnius, Lithuania
[4] Thermo Fisher Sci Balt, V A Graiciuno str 8, LT-02241 Vilnius, Lithuania
关键词
fusion transcripts; prostate cancer; RNA sequencing; TMPRSS2; transcriptomics; NEXT-GENERATION; GENE FUSIONS; TRANSCRIPTS; EXPRESSION; RNAS;
D O I
10.1002/1878-0261.13428
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Genetic rearrangements that fuse an androgen-regulated promoter area with a protein-coding portion of an originally androgen-unaffected gene are frequent in prostate cancer, with the fusion between transmembrane serine protease 2 (TMPRSS2) and ETS transcription factor ERG (ERG) (TMPRSS2-ERG fusion) being the most prevalent. Conventional hybridization- or amplification-based methods can test for the presence of expected gene fusions, but the exploratory analysis of currently unknown fusion partners is often cost-prohibitive. Here, we developed an innovative next-generation sequencing (NGS)-based approach for gene fusion analysis termed fusion sequencing via terminator-assisted synthesis (FTAS-seq). FTAS-seq can be used to enrich the gene of interest while simultaneously profiling the whole spectrum of its 30 -terminal fusion partners. Using this novel semi-targeted RNA-sequencing technique, we were able to identify 11 previously uncharacterized TMPRSS2 fusion partners and capture a range of TMPRSS2-ERG isoforms. We tested the performance of FTASseq with well-characterized prostate cancer cell lines and utilized the technique for the analysis of patient RNA samples. FTAS-seq chemistry combined with appropriate primer panels holds great potential as a tool for biomarker discovery that can support the development of personalized cancer therapies.
引用
收藏
页码:993 / 1006
页数:14
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