Octamerization enables soluble CD46 receptor to neutralize measles virus in vitro and in vivo.

نویسندگان

  • D Christiansen
  • P Devaux
  • B Réveil
  • A Evlashev
  • B Horvat
  • J Lamy
  • C Rabourdin-Combe
  • J H Cohen
  • D Gerlier
چکیده

A chimeric fusion protein encompassing the CD46 ectodomain linked to the C-terminal part of the C4b binding protein (C4bp) alpha chain (sCD46-C4bpalpha) was produced in eukaryotic cells. This protein, secreted as a disulfide-linked homo-octamer, was recognized by a panel of anti-CD46 antibodies with varying avidities. Unlike monomeric sCD46, the octameric sCD46-C4bpalpha protein was devoid of complement regulatory activity. However, sCD46-C4bpalpha was able to bind to the measles virus hemagglutinin protein expressed on murine cells with a higher avidity than soluble monomeric sCD46. Moreover, the octameric sCD46-C4bpalpha protein was significantly more efficient than monomeric sCD46 in inhibiting virus binding to CD46, in blocking virus induced cell-cell fusion, and in neutralizing measles virus in vitro. In addition, the octameric sCD46-C4bpalpha protein, but not the monomeric sCD46, fully protected CD46 transgenic mice against a lethal intracranial measles virus challenge.

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عنوان ژورنال:
  • Journal of virology

دوره 74 10  شماره 

صفحات  -

تاریخ انتشار 2000