Transfer of functional microRNAs between glioblastoma and microvascular endothelial cells through gap junctions

Dominique Thuringer, Jonathan Boucher, Gaetan Jego, Nicolas Pernet, Laurent Cronier, Arlette Hammann, Eric Solary, Carmen Garrido

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    43 Citations (Scopus)

    Abstract

    Extensive invasion and angiogenesis are hallmark features of malignant glioblastomas. Here, we co-cultured U87 human glioblastoma cells and human microvascular endothelial cells (HMEC) to demonstrate the exchange of microRNAs that initially involve the formation of gap junction communications between the two cell types. The functional inhibition of gap junctions by carbenoxolone blocks the transfer of the anti-tumor miR-145-5p from HMEC to U87, and the transfer of the pro-invasive miR-5096 from U87 to HMEC. These two microRNAs exert opposite effects on angiogenesis in vitro. MiR-5096 was observed to promote HMEC tubulogenesis, initially by increasing Cx43 expression and the formation of heterocellular gap junctions, and secondarily through a gap-junction independent pathway.Our results highlight the importance of microRNA exchanges between tumor and endothelial cells that in part involves the formation of functional gap junctions between the two cell types.

    Original languageEnglish
    Pages (from-to)73925-73934
    Number of pages10
    JournalOncotarget
    Volume7
    Issue number45
    DOIs
    Publication statusPublished - 1 Jan 2016

    Keywords

    • Connexin
    • Gap junction
    • Glioblastoma
    • MicroRNA
    • Tubulogenesis

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