Mechanism of HIV-1 Virion Entrapment by Tetherin

Tetherin,an interferon-inducible membrane protein,inhibits the release of nascent enveloped viral particles from the surface of infected cells. however,the mechanisms underlying virion retention have not yet been fully delineated. here,we employ biochemical assays and engineered tetherin proteins to demonstrate conclusively that virion tethers are composed of the tetherin protein itself,and to elucidate the configuration and topology that tetherin adopts during virion entrapment. we demonstrate that tetherin dimers adopt an axial configuration,in which pairs of transmembrane domains or pairs of glycosylphosphatidyl inositol anchors are inserted into assembling virion particles,while the remaining pair of membrane anchors remains embedded in the infected cell membrane. we use quantitative western blotting to determine that a few dozen tetherin dimers are used to tether each virion particle,and that there is ∼3- to 5-fold preference for the insertion of glycosylphosphatidyl inositol anchors rather than transmembrane domains into tethered virions. cumulatively,these results demonstrate that axially configured tetherin homodimers are directly responsible for trapping virions at the cell surface. we suggest that insertion of glycosylphosphatidyl inositol anchors may be preferred so that effector functions that require exposure of the tetherin n-terminus to the cytoplasm of infected cells are retained. © 2013 venkatesh,bieniasz.