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Organization of cellular receptors into a nanoscale junction during HIV-1 adhesion.


ABSTRACT: The fusion of the human immunodeficiency virus type 1 (HIV-1) with its host cell is the target for new antiretroviral therapies. Viral particles interact with the flexible plasma membrane via viral surface protein gp120 which binds its primary cellular receptor CD4 and subsequently the coreceptor CCR5. However, whether and how these receptors become organized at the adhesive junction between cell and virion are unknown. Here, stochastic modeling predicts that, regarding binding to gp120, cellular receptors CD4 and CCR5 form an organized, ring-like, nanoscale structure beneath the virion, which locally deforms the plasma membrane. This organized adhesive junction between cell and virion, which we name the viral junction, is reminiscent of the well-characterized immunological synapse, albeit at much smaller length scales. The formation of an organized viral junction under multiple physiopathologically relevant conditions may represent a novel intermediate step in productive infection.

SUBMITTER: Dobrowsky TM 

PROVIDER: S-EPMC2904768 | biostudies-literature | 2010 Jul

REPOSITORIES: biostudies-literature

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Organization of cellular receptors into a nanoscale junction during HIV-1 adhesion.

Dobrowsky Terrence M TM   Daniels Brian R BR   Siliciano Robert F RF   Sun Sean X SX   Wirtz Denis D  

PLoS computational biology 20100715 7


The fusion of the human immunodeficiency virus type 1 (HIV-1) with its host cell is the target for new antiretroviral therapies. Viral particles interact with the flexible plasma membrane via viral surface protein gp120 which binds its primary cellular receptor CD4 and subsequently the coreceptor CCR5. However, whether and how these receptors become organized at the adhesive junction between cell and virion are unknown. Here, stochastic modeling predicts that, regarding binding to gp120, cellula  ...[more]

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