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. 2012 Feb 12;18(3):382-4.
doi: 10.1038/nm.2673.

Identification of new ALK and RET gene fusions from colorectal and lung cancer biopsies

Affiliations

Identification of new ALK and RET gene fusions from colorectal and lung cancer biopsies

Doron Lipson et al. Nat Med. .

Abstract

Applying a next-generation sequencing assay targeting 145 cancer-relevant genes in 40 colorectal cancer and 24 non-small cell lung cancer formalin-fixed paraffin-embedded tissue specimens identified at least one clinically relevant genomic alteration in 59% of the samples and revealed two gene fusions, C2orf44-ALK in a colorectal cancer sample and KIF5B-RET in a lung adenocarcinoma. Further screening of 561 lung adenocarcinomas identified 11 additional tumors with KIF5B-RET gene fusions (2.0%; 95% CI 0.8-3.1%). Cells expressing oncogenic KIF5B-RET are sensitive to multi-kinase inhibitors that inhibit RET.

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Conflict of interest statement

COMPETING FINANCIAL INTERESTS

The authors declare competing financial interests: details accompany the full-text HTML version of the paper at http://www.nature.com/naturemedicine/.

Figures

Figure 1
Figure 1
DNA alterations identified in 40 CRC FFPE specimens. (a) The columns in the table denote samples, and the rows denote genes. A number inside the cell indicates the number of alterations of a specific type identified here. (b) A 5,194,955-bp tandem duplication generates an in-frame C2orf44-ALK gene fusion. (c) The RNA sequence of the C2orf44-ALK gene fusion shows aberrant splicing. UTR, untranslated region. (d) RNA sequencing shows an 89.8-fold increase in expression of ALK beginning at exon 20 relative to exons 1–19.
Figure 2
Figure 2
DNA alterations identified in 24 NSCLC FFPE specimens. (a) The columns in the table denote samples, and the rows denote genes. (b) An 11,294,741-bp inversion generates an in-frame KIF5B-RET gene fusion and the reciprocal RET-KIF5B fusion. (c) Protein domain structure of the RET-KIF5B and KIF5B-RET fusions. (d) RNA sequencing shows a 7.3-fold increase in expression of RET beginning at exon 12 relative to exons 1–11. (e) Focal moderate cytoplasmic immunoreactivity for RET protein expression (using avidin-biotin peroxidase). Scale bar, 100 μm; inset, 10 μm. (f) Ba/F3 cells with the KIF5B-REF fusion were treated with different drugs at the indicated concentrations, and viable cells were measured after 72 h of treatment and plotted relative to untreated controls. (g) Cells from e were treated with increasing concentrations of sunitinib or gefitinib for 6 h, and immunoblotting was used to detect the indicated proteins. Conc, concentration; pRET, phosphorylated RET.

Comment in

  • Genetics: Gene fusion power.
    Villanueva MT. Villanueva MT. Nat Rev Clin Oncol. 2012 Feb 28;9(4):188. doi: 10.1038/nrclinonc.2012.26. Nat Rev Clin Oncol. 2012. PMID: 22371133 No abstract available.
  • Chipping away at the lung cancer genome.
    Pao W, Hutchinson KE. Pao W, et al. Nat Med. 2012 Mar 6;18(3):349-51. doi: 10.1038/nm.2697. Nat Med. 2012. PMID: 22395697 No abstract available.

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