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Literature DB >> 31278449

Routine RNA sequencing of formalin-fixed paraffin-embedded specimens in neuropathology diagnostics identifies diagnostically and therapeutically relevant gene fusions.

Damian Stichel^1,2, Daniel Schrimpf^1,2, Belén Casalini^1,2, Jochen Meyer^1,2, Annika K Wefers^1,2,3, Philipp Sievers^1,2, Andrey Korshunov^1,2,3, Christian Koelsche^1,2,4, David E Reuss^1,2, Annekathrin Reinhardt^1,2, Azadeh Ebrahimi^1,2, Francisco Fernández-Klett^1,2, Tobias Kessler^5,6, Dominik Sturm^3,7,8, Jonas Ecker^3,8,9, Till Milde^3,8,9, Christel Herold-Mende¹⁰, Olaf Witt^3,8,9, Stefan M Pfister^3,7,8, Wolfgang Wick^5,6, David T W Jones^3,11, Andreas von Deimling^12,13, Felix Sahm^14,15,16.

Abstract

Molecular markers have become pivotal in brain tumor diagnostics. Mutational analyses by targeted next-generation sequencing of DNA and array-based DNA methylation assessment with copy number analyses are increasingly being used in routine diagnostics. However, the broad variety of gene fusions occurring in brain tumors is marginally covered by these technologies and often only assessed by targeted assays. Here, we assessed the feasibility and clinical value of investigating gene fusions in formalin-fixed paraffin-embedded (FFPE) tumor tissues by next-generation mRNA sequencing in a routine diagnostic setting. After establishment and optimization of a workflow applicable in a routine setting, prospective diagnostic application in a neuropathology department for 26 months yielded relevant fusions in 66 out of 101 (65%) analyzed cases. In 43 (43%) cases, the fusions were of decisive diagnostic relevance and in 40 (40%) cases the fusion genes rendered a druggable target. A major strength of this approach was its ability to detect fusions beyond the canonical alterations for a given entity, and the unbiased search for any fusion event in cases with uncertain diagnosis and, thus, uncertain spectrum of expected fusions. This included both rare variants of established fusions which had evaded prior targeted analyses as well as the detection of previously unreported fusion events. While the impact of fusion detection on diagnostics is highly relevant, it is especially the detection of "druggable" fusions which will most likely provide direct benefit to the patients. The wider application of this approach for unbiased fusion identification therefore promises to be a major advance in identifying alterations with immediate impact on patient care.

Entities: Chemical Disease Species

Keywords: Gene fusions; Molecular classification; Molecular diagnostics; RNA sequencing; Targeted treatment

Year: 2019 PMID： 31278449 DOI： 10.1007/s00401-019-02039-3

Source DB: PubMed Journal: Acta Neuropathol ISSN： 0001-6322 Impact factor: 17.088

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Cited

15 in total

1. Isomorphic diffuse glioma is a morphologically and molecularly distinct tumour entity with recurrent gene fusions of MYBL1 or MYB and a benign disease course.

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Journal: Acta Neuropathol Date: 2019-09-28 Impact factor: 17.088

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