4.2 Article

Concomitance of a novel RMDN2-ALK fusion and an EML4-ALK fusion in a lung adenocarcinoma

Journal

CANCER GENETICS
Volume 258, Issue -, Pages 18-22

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.cancergen.2021.06.004

Keywords

RMDN2-ALK fusion; EML4-ALK fusion; ALK rearrangements; Lung cancer; Next generation sequencing

Funding

  1. Johns Hopkins University School of Medicine

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This study identified a rare case of lung adenocarcinoma with two ALK fusions: a novel RMDN2-ALK fusion and a common EML4-ALK fusion. Multiple molecular assays were used to confirm the presence of these fusions and additional genomic rearrangements in the tumor.
The anaplastic lymphoma kinase (ALK) fusions/rearrangements in non-small cell lung cancer (NSCLC) act as oncogenic driver mutations. ALK tyrosine kinase inhibitors have anti-tumor activities in ALK-positive NSCLC. Although the EML4-ALK fusion is common in NSCLC, concomitance of an additional ALK fusion together with an EML4-ALK fusion is not common. Here, we present a lung adenocarcinoma with two ALK fusions, a novel RMDN2-ALK fusion accompanied by an EML4-ALK fusion, detected by a targeted next generation sequencing assay. The genomic translocation breakpoints of the RMDN2-ALK fusion were mapped to intron 2 for RMDN2 and exon 15 for ALK, and EML4-ALK breakpoints were mapped to intron 13 for EML4 and intron 19 for ALK. ALK break-apart FISH detected multiple ALK rearrangements, a gene fusion panel (NanoString) test confirmed the EML4-ALK fusion, and RNA-sequencing revealed two ALK fusions. The RMDN2 gene locates at the short arm of chromosome 2 between ALK and EML4 genes. The intact ALK kinase domain fused to RMDN2. Genome-wide copy number variants were found in multiple chromosome arms and the short arm of chromosome 2, suggestive of complex rearrangements. Further detailed analyses of breakpoints and copy number variants may shed light on mechanisms of their formation and pathogenesis in lung malignancies. (c) 2021 Elsevier Inc. All rights reserved.

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