HGF/SF induces mesothelial cell migration and proliferation by autocrine and paracrine pathways

Richard Warn, Pascale Harvey, Alba Warn, Adam Foley-Comer, Paraskevi Heldin, Marjan Versnel, Naokatu Arakaki, Yasushi Daikuhara, Geoffrey J. Laurent, Sarah E. Herrick, Steven E. Mutsaers

    Research output: Contribution to journalArticlepeer-review

    Abstract

    Mesothelial repair differs from that of other epithelial-like surfaces as healing does not occur solely by centripetal in-growth of cells as a sheet from the wound margins. Mesothelial cells lose their cell-cell junctions, divide, and adopt a fibroblast-like morphology while scattering across and covering the wound surface. These features are consistent with a cellular response to hepatocyte growth factor/scatter factor (HGF/SF). In this study, we examined the ability of mesothelial cells to secrete HGF/SF and investigated its possible role as an autocrine regulator of mesothelial cell motility and proliferation. We found that human primary mesothelial cells expressed HGF/SF mRNA and secreted active HGF/SF into conditioned medium as determined by ELISA and in a scattering bioassay. These cells also expressed the HGF/SF receptor, Met, as shown by RT-PCR and by Western blot analysis and immunofluorescence. Incubation of mesothelial cells with neutralizing antibodies to HGF/SF decreased cell migration to 25% of controls, whereas addition of HGF/SF disrupted cell-cell junctions and induced scattering and enhanced mesothelial cell migration. Furthermore, HGF/SF showed a small but significant mitogenic effect on all mesothelial cell lines examined. In conclusion, HGF/SF is produced by mesothelial cells and induces both motility and proliferation of these cells. These data are consistent with HGF/SF playing an autocrine role in mesothelial healing. © 2001 Academic Press.
    Original languageEnglish
    Pages (from-to)258-266
    Number of pages8
    JournalExperimental Cell Research
    Volume267
    Issue number2
    DOIs
    Publication statusPublished - 15 Jul 2001

    Keywords

    • Autocrine communication
    • Cell division
    • Chemotaxis
    • Hepatocyte growth factor
    • Mesothelium
    • Wound healing

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