Author: Acosta, Eliana G.; Castilla, Viviana; Damonte, Elsa B.
Title: Alternative infectious entry pathways for dengue virus serotypes into mammalian cells Cord-id: cn7sc03m Document date: 2009_6_11
ID: cn7sc03m
Snippet: The entry of two dengue virus (DENV) serotypes into Vero cells was analysed using biochemical inhibitors, dominant negative mutants of cellular proteins involved in endocytic pathways, fluorescence microscopy and infectivity determinations. By treatment with dansylcadaverine and chlorpromazine and overexpression of a dominant negative form of the Eps15 protein, a clathrinâ€mediated endocytosis for productive DENVâ€1 internalization into Vero cells was demonstrated whereas the infectious entry
Document: The entry of two dengue virus (DENV) serotypes into Vero cells was analysed using biochemical inhibitors, dominant negative mutants of cellular proteins involved in endocytic pathways, fluorescence microscopy and infectivity determinations. By treatment with dansylcadaverine and chlorpromazine and overexpression of a dominant negative form of the Eps15 protein, a clathrinâ€mediated endocytosis for productive DENVâ€1 internalization into Vero cells was demonstrated whereas the infectious entry of DENVâ€2 in the same cell system was independent of clathrin. Treatment with the inhibitors nystatin and methylâ€Î²â€cyclodextrin, as well as transfection of Vero cells with dominant negative caveolinâ€1, had no effect on DENVâ€2 virus infection. It was also shown, by using the K44A mutant and the inhibitor dynasore, that dynamin was required for DENVâ€2 entry. Consequently, the infectious entry of DENVâ€2 into Vero cells occurs by a nonâ€classical endocytic pathway independent of clathrin, caveolae and lipid rafts, but dependent on dynamin. By contrast, DENVâ€2 entry into A549 cells was clathrinâ€dependent, as previously reported in HeLa, C6/36 and BSâ€Câ€1 cells. Our results conclusively show, for the first time, a differential mode of infective entry for DENVâ€1 and DENVâ€2 into a common host cell, Vero cells, as well as alternative entry pathways for a given serotype, DENVâ€2, into different types of cells.
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