Role of Gag and lipids during HIV-1 assembly in CD4 T cells and Macrophages
HIV-1 is an RNA enveloped virus that preferentiallyinfects CD4+ T lymphocytes andalso macrophages. In CD4+ T cells, HIV-1mainly buds from the host cell plasma membrane.The viral Gag polyprotein targets theplasma membrane and is the orchestrator ofthe HIV assembly as its expression is sufficientto pr...
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doaj-0c9a1392685a4a0f8c4a4d0f6e5706052020-11-25T00:02:13ZengFrontiers Media S.A.Frontiers in Microbiology1664-302X2014-06-01510.3389/fmicb.2014.0031291478Role of Gag and lipids during HIV-1 assembly in CD4 T cells and MacrophagesCharlotte eMariani0Marion eDesdouits1Cyril eFavard2Philippe eBenaroch3Delphine M Muriaux4CNRS UMR5236Institut Curie - Inserm U932CNRS UMR5236Institut Curie - Inserm U932CNRS UMR5236HIV-1 is an RNA enveloped virus that preferentiallyinfects CD4+ T lymphocytes andalso macrophages. In CD4+ T cells, HIV-1mainly buds from the host cell plasma membrane.The viral Gag polyprotein targets theplasma membrane and is the orchestrator ofthe HIV assembly as its expression is sufficientto promote the formation of virus-likeparticles particles carrying a lipidic envelopederiving from the host cell membrane. Certainlipids are enriched in the viral membraneand are thought to play a key role in theassembly process and the envelop composition.A large body of work performed oninfected CD4+ T cells has provided importantknowledge about the assembly process andthe membrane virus lipid composition. WhileHIV assembly and budding in macrophages isthought to follow the same general Gag-drivenmechanism as in T-lymphocytes, the HIV cyclein macrophage exhibits specific features.In these cells, new virions bud from the limitingmembrane of seemingly intracellular compartments,where they accumulate while remaininginfectious. These structures are now oftenreferred to as Virus Containing Compartments(VCCs). Recent studies suggest that VCCsrepresent intracellularly sequestered regionsof the plasma membrane, but their precisenature remains elusive. The proteomic andlipidomic characterization of virions producedby T cells or macrophages has highlightedthe similarity between their composition andthat of the plasma membrane of producercells, as well as their enrichment in acidiclipids, some components of raft lipids andin tetraspanin-enriched microdomains. Greatchances are that Gag promotes the coalescenceof these components into an assemblyplatform from which viral budding takesplace. How Gag exactly interacts with membranelipids and what are the mechanisms involvedin the interaction between the differentmembrane nanodomains within the assemblyplatform remains unclear. Here we review recentliterature regarding the role of Gag andlipidshttp://journal.frontiersin.org/Journal/10.3389/fmicb.2014.00312/fullHIV-1LipidsMacrophagesGagAssemblyCD4 T-cells |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Charlotte eMariani Marion eDesdouits Cyril eFavard Philippe eBenaroch Delphine M Muriaux |
spellingShingle |
Charlotte eMariani Marion eDesdouits Cyril eFavard Philippe eBenaroch Delphine M Muriaux Role of Gag and lipids during HIV-1 assembly in CD4 T cells and Macrophages Frontiers in Microbiology HIV-1 Lipids Macrophages Gag Assembly CD4 T-cells |
author_facet |
Charlotte eMariani Marion eDesdouits Cyril eFavard Philippe eBenaroch Delphine M Muriaux |
author_sort |
Charlotte eMariani |
title |
Role of Gag and lipids during HIV-1 assembly in CD4 T cells and Macrophages |
title_short |
Role of Gag and lipids during HIV-1 assembly in CD4 T cells and Macrophages |
title_full |
Role of Gag and lipids during HIV-1 assembly in CD4 T cells and Macrophages |
title_fullStr |
Role of Gag and lipids during HIV-1 assembly in CD4 T cells and Macrophages |
title_full_unstemmed |
Role of Gag and lipids during HIV-1 assembly in CD4 T cells and Macrophages |
title_sort |
role of gag and lipids during hiv-1 assembly in cd4 t cells and macrophages |
publisher |
Frontiers Media S.A. |
series |
Frontiers in Microbiology |
issn |
1664-302X |
publishDate |
2014-06-01 |
description |
HIV-1 is an RNA enveloped virus that preferentiallyinfects CD4+ T lymphocytes andalso macrophages. In CD4+ T cells, HIV-1mainly buds from the host cell plasma membrane.The viral Gag polyprotein targets theplasma membrane and is the orchestrator ofthe HIV assembly as its expression is sufficientto promote the formation of virus-likeparticles particles carrying a lipidic envelopederiving from the host cell membrane. Certainlipids are enriched in the viral membraneand are thought to play a key role in theassembly process and the envelop composition.A large body of work performed oninfected CD4+ T cells has provided importantknowledge about the assembly process andthe membrane virus lipid composition. WhileHIV assembly and budding in macrophages isthought to follow the same general Gag-drivenmechanism as in T-lymphocytes, the HIV cyclein macrophage exhibits specific features.In these cells, new virions bud from the limitingmembrane of seemingly intracellular compartments,where they accumulate while remaininginfectious. These structures are now oftenreferred to as Virus Containing Compartments(VCCs). Recent studies suggest that VCCsrepresent intracellularly sequestered regionsof the plasma membrane, but their precisenature remains elusive. The proteomic andlipidomic characterization of virions producedby T cells or macrophages has highlightedthe similarity between their composition andthat of the plasma membrane of producercells, as well as their enrichment in acidiclipids, some components of raft lipids andin tetraspanin-enriched microdomains. Greatchances are that Gag promotes the coalescenceof these components into an assemblyplatform from which viral budding takesplace. How Gag exactly interacts with membranelipids and what are the mechanisms involvedin the interaction between the differentmembrane nanodomains within the assemblyplatform remains unclear. Here we review recentliterature regarding the role of Gag andlipids |
topic |
HIV-1 Lipids Macrophages Gag Assembly CD4 T-cells |
url |
http://journal.frontiersin.org/Journal/10.3389/fmicb.2014.00312/full |
work_keys_str_mv |
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