APOBEC3G Multimers Are Recruited to the Plasma Membrane for Packaging into Human Immunodeficiency Virus Type 1 Virus-Like Particles in an RNA-Dependent Process Requiring the NC Basic Linker

doi:10.1128/JVI.02237-06

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Journal of Virology, May 2007, p. 5000-5013, Vol. 81, No. 10
0022-538X/07/$08.00+0 doi:10.1128/JVI.02237-06
Copyright © 2007, American Society for Microbiology. All Rights Reserved.

APOBEC3G Multimers Are Recruited to the Plasma Membrane for Packaging into Human Immunodeficiency Virus Type 1 Virus-Like Particles in an RNA-Dependent Process Requiring the NC Basic Linker

Atuhani Burnett¹^,2 and Paul Spearman²^*

Department of Microbiology and Immunology, Vanderbilt University School of Medicine, Nashville, Tennessee,¹ Departments of Pediatrics and Microbiology and Immunology, Emory University School of Medicine, Atlanta, Georgia²

Received 11 October 2006/ Accepted 27 February 2007

APOBEC3G is an endogenous host restriction factor that inhibitshuman immunodeficiency virus (HIV) replication. The antiviralactivity of APOBEC3G is dependent upon its incorporation intothe virus particle. The mechanisms governing incorporation ofAPOBEC3G into virus particles are not completely understood.In particular, some investigators have reported that APOBEC3Ginteracts directly with the nucleocapsid (NC) subunit of Gag,while others have found that an RNA intermediate is requiredfor Gag-APOBEC3G interactions. In this study, we confirmed theRNA dependence of APOBEC3G packaging and performed detailedmapping of the determinants within NC that are required forvirion incorporation. Surprisingly, APOBEC3G packaging did notcorrelate well with the presence of the N-terminal "I," or interaction,domain within NC. Specifically, Gag constructs containing onlythe N-terminal region of NC packaged minimal amounts of APOBEC3G,while significant levels of APOBEC3G packaging were achievedwith Gag constructs containing the basic linker region of NC.Furthermore, membrane-binding experiments revealed that thebasic linker region was essential for the membrane associationof APOBEC3G in a Gag-APOBEC3G complex. Fluorescence resonanceenergy transfer was detected between labeled APOBEC3G in cellsand in particles, indicating that APOBEC3G is packaged as amultimer that is bound to packaged RNA. Regions of APOBEC3G-Gagcolocalization at the plasma membrane were detected that weredistinct from the punctate cytoplasmic bodies where APOBEC3Gaccumulates within the cell. Together, our results indicatethat APOBEC3G multimerizes in an RNA-dependent fashion and thatRNA-APOBEC3G multimers are recruited to the plasma membraneand subsequently into virion particles by Gag.

* Corresponding author. Mailing address: Pediatric Infectious Diseases, Emory University School of Medicine, 2015 Uppergate Dr., Atlanta, GA 30322. Phone: (404) 727-5642. Fax: (404) 727-8249. E-mail: paul_spearman{at}oz.ped.emory.edu

Published ahead of print on 7 March 2007.

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