| Literature DB >> 24632752 |
Kirsten D Mertz1, Gaurav Pathria2, Christine Wagner2, Juha Saarikangas3, Andrea Sboner4, Julia Romanov5, Melanie Gschaider5, Florian Lenz6, Friederike Neumann6, Wolfgang Schreiner6, Maria Nemethova7, Alexander Glassmann8, Pekka Lappalainen9, Georg Stingl5, J Victor Small7, Dieter Fink10, Lynda Chin11, Stephan N Wagner12.
Abstract
In cancers with a highly altered genome, distinct genetic alterations drive subsets rather than the majority of individual tumours. Here we use a sequential search across human tumour samples for transcript outlier data points with associated gene copy number variations that correlate with patient's survival to identify genes with pro-invasive functionality. Employing loss and gain of function approaches in vitro and in vivo, we show that one such gene, MTSS1, promotes the ability of melanocytic cells to metastasize and engages actin dynamics via Rho-GTPases and cofilin in this process. Indeed, high MTSS1 expression defines a subgroup of primary melanomas with unfavourable prognosis. These data underscore the biological, clinical and potential therapeutic implications of molecular subsets within genetically complex cancers.Entities:
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Year: 2014 PMID: 24632752 DOI: 10.1038/ncomms4465
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919