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Evolution and structure of clinically relevant gene fusions in multiple myeloma

Nature Communications, ISSN: 2041-1723, Vol: 11, Issue: 1, Page: 2666
2020
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3′ MACE RNA-sequencing allows for transcriptome profiling in human tissue samples after long-term storage

Researchers at the University of Freiburg aimed to compare the potential of standard RNA-sequencing (RNA-Seq) and 3′ massive analysis of c-DNA ends (MACE) RNA-sequencing for the analysis of fresh tissue and describe transcriptome profiling of formalin-fixed paraffin-embedded (FFPE) archival human samples by MACE. To compare MACE to standard RNA-Seq on fresh tissue, four healthy conjunctiva from fo

Article Description

Multiple myeloma is a plasma cell blood cancer with frequent chromosomal translocations leading to gene fusions. To determine the clinical relevance of fusion events, we detect gene fusions from a cohort of 742 patients from the Multiple Myeloma Research Foundation CoMMpass Study. Patients with multiple clinic visits enable us to track tumor and fusion evolution, and cases with matching peripheral blood and bone marrow samples allow us to evaluate the concordance of fusion calls in patients with high tumor burden. We examine the joint upregulation of WHSC1 and FGFR3 in samples with t(4;14)-related fusions, and we illustrate a method for detecting fusions from single cell RNA-seq. We report fusions at MYC and a neighboring gene, PVT1, which are related to MYC translocations and associated with divergent progression-free survival patterns. Finally, we find that 4% of patients may be eligible for targeted fusion therapies, including three with an NTRK1 fusion.

Bibliographic Details

Foltz, Steven M; Gao, Qingsong; Yoon, Christopher J; Sun, Hua; Yao, Lijun; Li, Yize; Jayasinghe, Reyka G; Cao, Song; King, Justin; Kohnen, Daniel R; Fiala, Mark A; Ding, Li; Vij, Ravi

Springer Science and Business Media LLC

Chemistry; Biochemistry, Genetics and Molecular Biology; Physics and Astronomy

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