2pjv: Difference between revisions

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==Overview==
==Overview==
A thorough understanding of the structure of fusion domains of enveloped, viruses in changing lipid environments helps us to formulate mechanistic, models on how they might function in mediating viral entry by membrane, fusion. We have expressed the N-terminal fusion domain of HIV-1 gp41 as a, construct that is water-soluble in the absence of membranes, but that also, binds with high affinity to lipid micelles and bilayers in their presence., We have solved the structure and studied the dynamics of this domain bound, to dodecylphosphocholine micelles by homo- and heteronuclear NMR, spectroscopy. The fusion peptide forms a stable hydrophobic helix from, Ile(4) to Ala(14), but is increasingly more disordered and dynamic in a, segment of intermediate polarity that stretches from Ala(15) to Ser(23)., When bound to lipid bilayers at low concentration, the HIV fusion domain, is also largely alpha-helical, as determined by CD and FTIR spectroscopy., However, at higher protein/lipid ratios, the domain is partially converted, to form beta-structures in lipid bilayers. Controlled lipid mixing occurs, at concentrations that support the alpha-helical, but not the beta-strand, conformation.
A thorough understanding of the structure of fusion domains of enveloped viruses in changing lipid environments helps us to formulate mechanistic models on how they might function in mediating viral entry by membrane fusion. We have expressed the N-terminal fusion domain of HIV-1 gp41 as a construct that is water-soluble in the absence of membranes, but that also binds with high affinity to lipid micelles and bilayers in their presence. We have solved the structure and studied the dynamics of this domain bound to dodecylphosphocholine micelles by homo- and heteronuclear NMR spectroscopy. The fusion peptide forms a stable hydrophobic helix from Ile(4) to Ala(14), but is increasingly more disordered and dynamic in a segment of intermediate polarity that stretches from Ala(15) to Ser(23). When bound to lipid bilayers at low concentration, the HIV fusion domain is also largely alpha-helical, as determined by CD and FTIR spectroscopy. However, at higher protein/lipid ratios, the domain is partially converted to form beta-structures in lipid bilayers. Controlled lipid mixing occurs at concentrations that support the alpha-helical, but not the beta-strand conformation.


==About this Structure==
==About this Structure==
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[[Category: Single protein]]
[[Category: Single protein]]
[[Category: Li, Y]]
[[Category: Li, Y]]
[[Category: Tamm, L.K.]]
[[Category: Tamm, L K.]]
[[Category: domain]]
[[Category: domain]]
[[Category: dpc]]
[[Category: dpc]]
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[[Category: virus]]
[[Category: virus]]


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Revision as of 19:30, 21 February 2008

File:2pjv.gif


2pjv

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solution structure of hiv-1 gp41 fusion domain bound to DPC micelle

OverviewOverview

A thorough understanding of the structure of fusion domains of enveloped viruses in changing lipid environments helps us to formulate mechanistic models on how they might function in mediating viral entry by membrane fusion. We have expressed the N-terminal fusion domain of HIV-1 gp41 as a construct that is water-soluble in the absence of membranes, but that also binds with high affinity to lipid micelles and bilayers in their presence. We have solved the structure and studied the dynamics of this domain bound to dodecylphosphocholine micelles by homo- and heteronuclear NMR spectroscopy. The fusion peptide forms a stable hydrophobic helix from Ile(4) to Ala(14), but is increasingly more disordered and dynamic in a segment of intermediate polarity that stretches from Ala(15) to Ser(23). When bound to lipid bilayers at low concentration, the HIV fusion domain is also largely alpha-helical, as determined by CD and FTIR spectroscopy. However, at higher protein/lipid ratios, the domain is partially converted to form beta-structures in lipid bilayers. Controlled lipid mixing occurs at concentrations that support the alpha-helical, but not the beta-strand conformation.

About this StructureAbout this Structure

2PJV is a Single protein structure of sequence from Human immunodeficiency virus 1. Full crystallographic information is available from OCA.

ReferenceReference

Structure and plasticity of the human immunodeficiency virus gp41 fusion domain in lipid micelles and bilayers., Li Y, Tamm LK, Biophys J. 2007 Aug 1;93(3):876-85. Epub 2007 May 18. PMID:17513369

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