Literature DB >> 23099087

Elements in HIV-1 Gag contributing to virus particle assembly.

Ina P O'Carroll1, Ferri Soheilian, Anne Kamata, Kunio Nagashima, Alan Rein.   

Abstract

The Gag polyprotein is the building block of retroviral particles and its expression is sufficient for assembly in cells. In n class="Species">HIV-1, nucleic acid (NA) is required for recombinant Gag molecules to assemble in a defined system in vitro. Experiments performed by Barklis and co-workers suggested that NA contributes to assembly by promoting Gag oligomerization. Gag is composed of four main domains: the matrix (MA), capsid (CA), nucleocapsid (NC), and p6 domains. We have recently shown that the SP1 linker, which lies between the CA and NC domains, assumes a helical structure at high, but not low, concentrations. We suggested that Gag oligomerization mediates assembly via an SP1-dependent conformational switch that exposes new interfaces for assembly. Although NA is required for assembly in vitro, deletion of NC, the main RNA-binding domain, does not eliminate particle formation in vivo; these particles lack NA. We hypothesized that alternative pathways that lead to Gag oligomerization or an increase in local Gag concentration, namely Gag-membrane or inter-protein interactions, rescue assembly in the absence of NC-RNA binding. We constructed mutants in which either Gag-membrane binding, the Gag dimer interface, or NC-RNA binding are disrupted. None of these mutants disables assembly. However, combined mutations in any two of these three classes render Gag completely unable to form virus-like particles. Thus, it seems, Gag utilizes at least three types of interactions to form oligomers and any two out of the three are sufficient for assembly. Published by Elsevier B.V.

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Year:  2012        PMID: 23099087      PMCID: PMC6771925          DOI: 10.1016/j.virusres.2012.10.016

Source DB:  PubMed          Journal:  Virus Res        ISSN: 0168-1702            Impact factor:   3.303


  20 in total

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2.  Effect of multimerization on membrane association of Rous sarcoma virus and HIV-1 matrix domain proteins.

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4.  Atomic Modeling of an Immature Retroviral Lattice Using Molecular Dynamics and Mutagenesis.

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Review 7.  HIV-1 Gag as an Antiviral Target: Development of Assembly and Maturation Inhibitors.

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Journal:  Curr Top Med Chem       Date:  2016       Impact factor: 3.295

Review 8.  Retroviral Gag protein-RNA interactions: Implications for specific genomic RNA packaging and virion assembly.

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Journal:  Semin Cell Dev Biol       Date:  2018-04-01       Impact factor: 7.727

9.  Hydrodynamic and Membrane Binding Properties of Purified Rous Sarcoma Virus Gag Protein.

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10.  3D molecular models of whole HIV-1 virions generated with cellPACK.

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