Thu, 21 Aug 2008 21:41:54 BST CiteULike: di kieran101 Popov http://www.citeulike.org/user/kieran101/author/Popov CiteULike.org en-gb Copyright © 2004-2008 citeulike.org http://www.citeulike.org/user/kieran101/article/2802098 <i>J. Virol., Vol. 82, No. 10. (15 May 2008), pp. 4898-4907.</i><br /><br />To exit infected cells, human immunodeficiency virus type 1 (HIV-1) exploits the vacuolar protein-sorting pathway by engaging Tsg101 and ALIX through PTAP and LYPxnL late assembly (L) domains. In contrast, less-complex retroviruses often use PPxY L domains to recruit Nedd4 family ubiquitin ligases. Although HIV-1 Gag lacks PPxY motifs, we now show that the budding of various HIV-1 L-domain mutants is dramatically enhanced by ectopic Nedd4-2s, a native isoform with a truncated C2 domain. The effect of Nedd4-2s on HIV-1 budding required a catalytically active HECT domain and was specific, since other Nedd4 family proteins showed little activity and an unrelated retrovirus was not rescued. The residual C2 domain of Nedd4-2s was critical for the enhancement of HIV-1 budding and for the association of Nedd4-2s with Gag, as reflected by its incorporation into virus-like particles. Interestingly, the incorporation of Nedd4-2s also depended on its active site, indicating that the ability to form a thioester with ubiquitin was required. These data suggest a novel mechanism by which HIV-1 Gag can connect to cellular budding machinery. 10.1128/JVI.02675-07 Efficient and Specific Rescue of Human Immunodeficiency Virus Type 1 Budding Defects by a Nedd4-Like Ubiquitin Ligase Yoshiko Usami Sergei Popov Elena Popova Heinrich Gottlinger doi:10.1128/JVI.02675-07 J. Virol., Vol. 82, No. 10. (15 May 2008), pp. 4898-4907. 2008-05-15T16:23:02-00:00 2008 J. Virol. 82 10 4898 4907 budding ubiquitin