Bundles Consisting of Extended Transmembrane Segments of Vpu from HIV-1:  Computer Simulations and Conductance Measurements

Cordes, Frank; Tustian, A. D.; Sansom, Mark S. P.; Watts, A; Fischer, Wolfgang B.

doi:10.1021/bi025518p

Cited by 47 publications

(67 citation statements)

References 48 publications

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“…Comparable stability for structurally diverse oligomers in bilayers may explain experimental observations of multiple conductance levels for Vpu ion channels. 1,10,[13][14][15] Given that a variety of Vpu 1-40 oligomer structures coexist in DOPC/DOPG bilayers, we can not analyze our solid-state NMR data unequivocally in terms of a single structure. However, the fact that 2D 13 C-13 C spectra of Vpu in bilayers show a single set of 13 C chemical shifts 17 suggests that peptide conformations and intermolecular interactions in the predominant oligomers are similar.…”

Section: Discussionmentioning

confidence: 99%

“…Rather different pentamer models were used in simulations by Pertagias et al, 32 Grice et al, 25 and Cordes et al 10 In these simulations, helix orientations were chosen such that the side chain of S23 was located in the central pore, with the assumption that such an orientation would be thermodynamically preferred. Using our definition of the helix rotation angle, such models have q % 150 and do not fit our 2D CHHC and DIPSHIFT data.…”

Section: Discussionmentioning

confidence: 99%

“…9 The second function depends principally on the single transmembrane TM segment of Vpu, contained within residues 1-30, as sequence alterations in the TM segment have been shown to interfere with this function. 2 Full-length Vpu and various N-terminal peptides containing the TM segment have been shown to form cation-selective channels in model membranes 1,[10][11][12][13][14][15] and in cells. 12 These ion channels presumably form by association of a-helical TM segments into homo-oligomeric bundles, with ions passing through the central pore of the helix bundle.…”

Section: Introductionmentioning

confidence: 99%

“…17 Computational modeling of oligomers of Vpu TM segments has been carried out by several groups, resulting in detailed models for tetramers, pentamers, and hexamers. 10,[24][25][26][27][28][29] Predictions of channel conductance based on these models favor a pentamer or larger oligomer as the predominant channel. 10,25 Computational studies include investigations of interactions of channel-blocking compounds with Vpu ion channels, 30 effects of site-specific mutations on secondary structure and supramolecular structure, 31 and channel selectivity.…”

Section: Introductionmentioning

confidence: 99%

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Oligomerization state and supramolecular structure of the HIV‐1 Vpu protein transmembrane segment in phospholipid bilayers

et al. 2010

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HIV-1 Vpu is an 81-residue protein with a single N-terminal transmembrane (TM) helical segment that is involved in the release of new virions from host cell membranes. Vpu and its TM segment form ion channels in phospholipid bilayers, presumably by oligomerization of TM helices into a pore-like structure. We describe measurements that provide new constraints on the oligomerization state and supramolecular structure of residues 1-40 of Vpu (Vpu 1-40 ), including analytical ultracentrifugation measurements to investigate oligomerization in detergent micelles, photo-induced crosslinking experiments to investigate oligomerization in bilayers, and solid-state nuclear magnetic resonance measurements to obtain constraints on intermolecular contacts between and orientations of TM helices in bilayers. From these data, we develop molecular models for Vpu TM oligomers. The data indicate that a variety of oligomers coexist in phospholipid bilayers, so that a unique supramolecular structure can not be defined. Nonetheless, since oligomers of various sizes have similar intermolecular contacts and orientations, molecular models developed from our data are most likely representative of Vpu TM oligomers that exist in host cell membranes.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Oligomerization state and supramolecular structure of the HIV‐1 Vpu protein transmembrane segment in phospholipid bilayers

et al. 2010

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“…These structures suggest the lumen of the pore to be a widely hydrophobic stretch. Model 4 is similar to the one used so far in MD simulations with the TM part of Vpu, 11,49,50 whereas model 1 corresponds to a model which has been suggested earlier. 7,10 In the former model Ser-24 points into the pore, while in the latter it is Trp-23.…”

Section: Discussionmentioning

confidence: 99%

Assembly of Viral Membrane Proteins

Krüger¹,

Fischer²

2009

J. Chem. Theory Comput.

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Abstract:The generation of computational models is an alternative route to obtain reliable structures for the oligomeric state of membrane proteins. A strategy has been developed to search the conformational space of all possible assemblies in a reasonable time, taking symmetry considerations into account. The methodology tested on M2 from influenza A, shows an excellent agreement with established structures. For Vpu from HIV-1 a series of conformational distinct structures are proposed. For the first time a structural model for a fully assembled transmembrane part of 3a from SARSCoV is proposed.

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Assembling viral channel forming proteins: Vpu from HIV‐1

Li¹,

Hsu²,

Fischer³

2013

Biopolymers

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Different routes of assembly are probed for the transmembrane domain (TMD) of the bitopic membrane protein Vpu from HIV-1. Vpu is responsible for the amplification of viral release from the host cell. The mode of action includes (i) heteroassembly with host factors and (ii) the formation of homo-oligomers, which are able to conduct ions across the lipid membrane. Two different routes of assembling short sequences of the N terminus, including the TMD of Vpu, Vpu1-32, and Vpu8-26, are presented by using a combination of classical molecular dynamics (MD) simulations combined with a docking approach. The rim of alanines (Ala-8, -11, -15, and -19) resembles an interlocking motif for the sequential assembly into a dimer and trimer. Simultaneous assembly results in oligomeric bundles (trimers to pentamers) with either tryptophans (Trp-23) or purely hydrophobic residues facing the center. Bundles, with serines facing the pore (Ser-24), are energetically not the lowest structures. For pentameric bundles with Ser-24 facing the pore, no water column develops during a short 25 ns MD simulation.

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Bundles Consisting of Extended Transmembrane Segments of Vpu from HIV-1: Computer Simulations and Conductance Measurements

Cited by 47 publications

References 48 publications

Oligomerization state and supramolecular structure of the HIV‐1 Vpu protein transmembrane segment in phospholipid bilayers

Oligomerization state and supramolecular structure of the HIV‐1 Vpu protein transmembrane segment in phospholipid bilayers

Assembly of Viral Membrane Proteins

Assembling viral channel forming proteins: Vpu from HIV‐1

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