2009
DOI: 10.1038/nchembio.268
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HIV-1 Nef membrane association depends on charge, curvature, composition and sequence

Abstract: Nef-mediated internalization of T-cell receptor molecules from the surface of an infected cell is required for the pathogenicity of HIV and disease progression to AIDS. This function depends on the N-terminal myristoylation of Nef, a lipid modification that targets the protein to membranes. We have analyzed how specific membrane properties and sequence motifs within Nef determine this interaction. Using time-resolved techniques we find that the association with membranes is a biphasic process with a fast rate … Show more

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Cited by 87 publications
(90 citation statements)
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References 48 publications
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“…Nef induces a number of genes involved in cholesterol synthesis ( 8,9 ) and can facilitate cholesterol delivery to lipid rafts ( 8,10 ). This activity is consistent with membrane localization of Nef due to myristoylation ( 8,11,12 ); nonmyristoylated Nef did not affect lipid rafts ( 8 ). Lipid rafts are the preferential sites of HIV-1 assembly and budding, and cholesterol content of lipid rafts determines the cholesterol content of virions, which is critical for virion infectivity.…”
Section: Lipid Raft Cholesterol Content Analysismentioning
confidence: 53%
“…Nef induces a number of genes involved in cholesterol synthesis ( 8,9 ) and can facilitate cholesterol delivery to lipid rafts ( 8,10 ). This activity is consistent with membrane localization of Nef due to myristoylation ( 8,11,12 ); nonmyristoylated Nef did not affect lipid rafts ( 8 ). Lipid rafts are the preferential sites of HIV-1 assembly and budding, and cholesterol content of lipid rafts determines the cholesterol content of virions, which is critical for virion infectivity.…”
Section: Lipid Raft Cholesterol Content Analysismentioning
confidence: 53%
“…In general this effect does not depend on the presence or absence of a membrane anchor, as a similar effect was found for all PrP variants in interactions with POPG liposomes. Based on this observation a direct interaction of the PrP N-terminal region with phospholipid membranes always occurs, as described for other lipid-anchored proteins such as Src proteins and HIV-1 Gag protein (27,44). However, tryptophan fluorescence quenching occurred to a different extent for PrPs with a membrane anchor compared with PrPs without a membrane anchor.…”
Section: Scmentioning
confidence: 96%
“…This is the case of the HIV viral protein Gag, whose myristoylation is critical for the formation of the viral capsid [39]. Similarly, the Nef protein, essential for viral replication, high virus load and progression to acquired immunodeficiency syndrome (AIDS), requires membrane association via myristoylation to exert its functions [40]. This together with the fact that myristoylation is misregulated in many other diseases (cancer, [41] neurological disorders [42]) has supported NMT as a potential therapeutical target.…”
Section: N-myristoylationmentioning
confidence: 99%