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      Gene fusions in soft tissue tumors: Recurrent and overlapping pathogenetic themes.

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          Abstract

          Gene fusions have been described in approximately one-third of soft tissue tumors (STT); of the 142 different fusions that have been reported, more than half are recurrent in the same histologic subtype. These gene fusions constitute pivotal driver mutations, and detailed studies of their cellular effects have provided important knowledge about pathogenetic mechanisms in STT. Furthermore, most fusions are strongly associated with a particular histotype, serving as ideal molecular diagnostic markers. In recent years, it has also become apparent that some chimeric proteins, directly or indirectly, constitute excellent treatment targets, making the detection of gene fusions in STT ever more important. Indeed, pharmacological treatment of STT displaying fusions that activate protein kinases, such as ALK and ROS1, or growth factors, such as PDGFB, is already in clinical use. However, the vast majority (52/78) of recurrent gene fusions create structurally altered and/or deregulated transcription factors, and a small but growing subset develops through rearranged chromatin regulators. The present review provides an overview of the spectrum of currently recognized gene fusions in STT, and, on the basis of the protein class involved, the mechanisms by which they exert their oncogenic effect are discussed.

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          Author and article information

          Journal
          Genes Chromosomes Cancer
          Genes, chromosomes & cancer
          Wiley-Blackwell
          1098-2264
          1045-2257
          Apr 2016
          : 55
          : 4
          Affiliations
          [1 ] Department of Clinical Genetics, University and Regional Laboratories, Lund University, Lund, Sweden.
          [2 ] Department of Pathology, Memorial Sloan Kettering Cancer Center, New York, NY.
          Article
          NIHMS811594
          10.1002/gcc.22335
          5012284
          26684580
          2b39c195-fc91-4658-9bfb-0c794e885cc5
          History

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