| Literature DB >> 24445538 |
Thomas Wiesner1,2, Jie He3, Roman Yelensky3, Rosaura Esteve-Puig4, Thomas Botton4, Iwei Yeh4, Doron Lipson3, Geoff Otto3, Kristina Brennan3, Rajmohan Murali1,5, Maria Garrido4, Vincent A Miller3, Jeffrey S Ross3, Michael F Berger1, Alyssa Sparatta4, Gabriele Palmedo6, Lorenzo Cerroni2, Klaus J Busam1, Heinz Kutzner6, Maureen T Cronin3, Philip J Stephens3, Boris C Bastian1,4,5.
Abstract
Spitzoid neoplasms are a group of melanocytic tumours with distinctive histopathological features. They include benign tumours (Spitz naevi), malignant tumours (spitzoid melanomas) and tumours with borderline histopathological features and uncertain clinical outcome (atypical Spitz tumours). Their genetic underpinnings are poorly understood, and alterations in common melanoma-associated oncogenes are typically absent. Here we show that spitzoid neoplasms harbour kinase fusions of ROS1 (17%), NTRK1 (16%), ALK (10%), BRAF (5%) and RET (3%) in a mutually exclusive pattern. The chimeric proteins are constitutively active, stimulate oncogenic signalling pathways, are tumourigenic and are found in the entire biologic spectrum of spitzoid neoplasms, including 55% of Spitz naevi, 56% of atypical Spitz tumours and 39% of spitzoid melanomas. Kinase inhibitors suppress the oncogenic signalling of the fusion proteins in vitro. In summary, kinase fusions account for the majority of oncogenic aberrations in spitzoid neoplasms and may serve as therapeutic targets for metastatic spitzoid melanomas.Entities:
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Year: 2014 PMID: 24445538 PMCID: PMC4084638 DOI: 10.1038/ncomms4116
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919