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Human Nucleoporins Promote HIV-1 Docking at the Nuclear Pore,Nuclear Import and Integration
Authors:Francesca Di Nunzio  Anne Danckaert  Thomas Fricke  Patricio Perez  Juliette Fernandez  Emmanuelle Perret  Pascal Roux  Spencer Shorte  Pierre Charneau  Felipe Diaz-Griffero  Nathalie J. Arhel
Affiliation:1. Molecular Virology and Vaccinology Unit, CNRS URA 3015, Department of Virology, Institut Pasteur, Paris, France.; 2. Imagopole, Institut Pasteur, Paris, France.; 3. Department of Microbiology and Immunology, Albert Einstein College of Medicine, Bronx, New York, United States of America.; University of South Carolina School of Medicine, United States of America,
Abstract:The nuclear pore complex (NPC) mediates nucleo-cytoplasmic transport of macromolecules and is an obligatory point of passage and functional bottleneck in the replication of some viruses. The Human Immunodeficiency Virus (HIV) has evolved the required mechanisms for active nuclear import of its genome through the NPC. However the mechanisms by which the NPC allows or even assists HIV translocation are still unknown. We investigated the involvement of four key nucleoporins in HIV-1 docking, translocation, and integration: Nup358/RanBP2, Nup214/CAN, Nup98 and Nup153. Although all induce defects in infectivity when depleted, only Nup153 actually showed any evidence of participating in HIV-1 translocation through the nuclear pore. We show that Nup358/RanBP2 mediates docking of HIV-1 cores on NPC cytoplasmic filaments by interacting with the cores and that the C-terminus of Nup358/RanBP2 comprising a cyclophilin-homology domain contributes to binding. We also show that Nup214/CAN and Nup98 play no role in HIV-1 nuclear import per se: Nup214/CAN plays an indirect role in infectivity read-outs through its effect on mRNA export, while the reduction of expression of Nup98 shows a slight reduction in proviral integration. Our work shows the involvement of nucleoporins in diverse and functionally separable steps of HIV infection and nuclear import.
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