Author: Merinoâ€Gracia, Javier; GarcÃaâ€Mayoral, MarÃa F.; RodrÃguezâ€Crespo, Ignacio
Title: The association of viral proteins with host cell dynein components during virus infection Cord-id: efi8s46k Document date: 2011_8_8
ID: efi8s46k
Snippet: After fusion with the cellular plasma membrane or endosomal membranes, viral particles are generally too large to diffuse freely within the crowded cytoplasm environment. Thus, they will never reach the cell nucleus or the perinuclear areas where replication or reverse transcription usually takes place. It has been proposed that many unrelated viruses are transported along microtubules in a retrograde manner using the cellular dynein machinery or, at least, some dynein components. A putative emp
Document: After fusion with the cellular plasma membrane or endosomal membranes, viral particles are generally too large to diffuse freely within the crowded cytoplasm environment. Thus, they will never reach the cell nucleus or the perinuclear areas where replication or reverse transcription usually takes place. It has been proposed that many unrelated viruses are transported along microtubules in a retrograde manner using the cellular dynein machinery or, at least, some dynein components. A putative employment of the dynein motor in a dyneinâ€mediated transport has been suggested from experiments in which viral capsid proteins were used as bait in yeast twoâ€hybrid screens using libraries composed of cellular proteins and dyneinâ€associated chains were retrieved as virusâ€interacting proteins. In most cases DYNLL1, DYNLT1 or DYNLRB1 were identified as the dynein chains that interact with viral proteins. The importance of these dynein–virus interactions has been supported, in principle, by the observation that in some cases the dyneinâ€interacting motifs of viral proteins altered by siteâ€directed mutagenesis result in nonâ€infective virions. Furthermore, overexpression of p50 dynamitin, which blocks the dynein–dynactin interaction, or incubation of infected cells with peptides that compete with viral polypeptides for dynein binding have been shown to alter the viral retrograde transport. Still, it remains to be proved that dynein light chains can bind simultaneously to incoming virions and to the dynein motor for retrograde transport to take place. In this review, we will analyse the association of viral proteins with dynein polypeptides and its implications for viral infection.
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