Literature DB >> 23878195

Interaction of transportin-SR2 with Ras-related nuclear protein (Ran) GTPase.

Oliver Taltynov1, Jonas Demeulemeester, Frauke Christ, Stéphanie De Houwer, Vicky G Tsirkone, Melanie Gerard, Stephen D Weeks, Sergei V Strelkov, Zeger Debyser.   

Abstract

The human immunodeficiency virus type 1 (HIV-1) and other lentiviruses are capable of infecting non-dividing cells and, therefore, need to be imported into the nucleus before integration into the host cell chromatin. Transportin-SR2 (TRN-SR2, Transportin-3, TNPO3) is a cellular karyopherin implicated in nuclear import of HIV-1. A model in which TRN-SR2 imports the viral preintegration complex into the nucleus is supported by direct interaction between TRN-SR2 and HIV-1 integrase (IN). Residues in the C-terminal domain of HIV-1 IN that mediate binding to TRN-SR2 were recently delineated. As for most nuclear import cargoes, the driving force behind HIV-1 preintegration complex import is likely a gradient of the GDP- and GTP-bound forms of Ran, a small GTPase. In this study we offer biochemical and structural characterization of the interaction between TRN-SR2 and Ran. By size exclusion chromatography we demonstrate stable complex formation of TRN-SR2 and RanGTP in solution. Consistent with the behavior of normal nuclear import cargoes, HIV-1 IN is released from the complex with TRN-SR2 by RanGTP. Although in concentrated solutions TRN-SR2 by itself was predominantly present as a dimer, the TRN-SR2-RanGTP complex was significantly more compact. Further analysis supported a model wherein one monomer of TRN-SR2 is bound to one monomer of RanGTP. Finally, we present a homology model of the TRN-SR2-RanGTP complex that is in excellent agreement with the experimental small angle x-ray scattering data.

Entities:  

Keywords:  GTPase; HIV-1; Homology Modeling; Host-Pathogen Interactions; Nuclear Transport; Protein-Protein Interactions; X-ray Scattering

Mesh:

Substances:

Year:  2013        PMID: 23878195      PMCID: PMC3757221          DOI: 10.1074/jbc.M113.484345

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  62 in total

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