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Data from MET Overexpression Turns Human Primary Osteoblasts into Osteosarcomas

Posted on 2023-03-30 - 17:09
Abstract

The MET oncogene was causally involved in the pathogenesis of a rare tumor, i.e., the papillary renal cell carcinoma, in which activating mutations, either germline or somatic, were identified. MET activating mutations are rarely found in other human tumors, whereas at higher frequencies, MET is amplified and/or overexpressed in sporadic tumors of specific histotypes, including osteosarcoma. In this work, we provide experimental evidence that overexpression of the MET oncogene causes and sustains the full-blown transformation of osteoblasts. Overexpression of MET, obtained by lentiviral vector–mediated gene transfer, resulted in the conversion of primary human osteoblasts into osteosarcoma cells, displaying the transformed phenotype in vitro and the distinguishing features of human osteosarcomas in vivo. These included atypical nuclei, aberrant mitoses, production of alkaline phosphatase, secretion of osteoid extracellular matrix, and striking neovascularization. Although with a lower tumorigenicity, this phenotype was superimposable to that observed after transfer of the MET gene activated by mutation. Both transformation and tumorigenesis were fully abrogated when MET expression was quenched by short-hairpin RNA or when signaling was impaired by a dominant-negative MET receptor. These data show that MET overexpression is oncogenic and that it is essential for the maintenance of the cancer phenotype. (Cancer Res 2006; 66(9): 4750-7)

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AUTHORS (14)

  • Salvatore Patanè
    Sofia Avnet
    Nadia Coltella
    Barbara Costa
    Simone Sponza
    Martina Olivero
    Elisa Vigna
    Luigi Naldini
    Nicola Baldini
    Riccardo Ferracini
    Simona Corso
    Silvia Giordano
    Paolo M. Comoglio
    Maria Flavia Di Renzo

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