Literature DB >> 17766368

Conformational changes induced by a single amino acid substitution in the trans-membrane domain of Vpu: implications for HIV-1 susceptibility to channel blocking drugs.

Sang Ho Park1, Stanley J Opella.   

Abstract

The channel-forming trans-membrane domain of Vpu (Vpu TM) from HIV-1 is known to enhance virion release from the infected cells and is a potential target for ion-channel blockers. The substitution of alanine at position 18 by a histidine (A18H) has been shown to render HIV-1 infections susceptible to rimantadine, a channel blocker of M2 protein from the influenza virus. In order to describe the influence of the mutation on the structure and rimantadine susceptibility of Vpu, we determined the structure of A18H Vpu TM, and compared it to those of wild-type Vpu TM and M2 TM. Both isotropic and orientationally dependent NMR frequencies of the backbone amide resonance of His18 were perturbed by rimantadine, and those of Ile15 and Trp22 were also affected, suggesting that His18 is the key residue for rimantadine binding and that residues located on the same face of the TM helix are also involved. A18H Vpu TM has an ideal, straight alpha-helix spanning residues 6-27 with an average tilt angle of 41 degrees in C14 phospholipid bicelles, indicating that the tilt angle is increased by 11 degrees compared to that of wild-type Vpu TM. The longer helix formed by the A18H mutation has a larger tilt angle to compensate for the hydrophobic mismatch with the length of the phospholipids in the bilayer. These results demonstrate that the local change of the primary structure plays an important role in secondary and tertiary structures of Vpu TM in lipid bilayers and affects its ability to interact with channel blockers.

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Year:  2007        PMID: 17766368      PMCID: PMC2204142          DOI: 10.1110/ps.073041107

Source DB:  PubMed          Journal:  Protein Sci        ISSN: 0961-8368            Impact factor:   6.725


  73 in total

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2.  Rotational diffusion of membrane proteins in aligned phospholipid bilayers by solid-state NMR spectroscopy.

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Review 4.  Solid-state NMR in drug design and discovery for membrane-embedded targets.

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Authors:  Sang Ho Park; Stanley J Opella
Journal:  J Mol Biol       Date:  2005-07-08       Impact factor: 5.469

6.  Functional domains within the human immunodeficiency virus type 2 envelope protein required to enhance virus production.

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Review 9.  Structural biology of HIV.

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  19 in total

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7.  NMR Structural Studies of Antimicrobial Peptides: LPcin Analogs.

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Review 8.  Magic angle spinning NMR of viruses.

Authors:  Caitlin M Quinn; Manman Lu; Christopher L Suiter; Guangjin Hou; Huilan Zhang; Tatyana Polenova
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Review 9.  NMR structures of membrane proteins in phospholipid bilayers.

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10.  NMR studies of p7 protein from hepatitis C virus.

Authors:  Gabriel A Cook; Stanley J Opella
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