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doi:10.1016/j.virol.2004.08.025 
Copyright © 2004 Elsevier Inc. All rights reserved.
Conserved residues in the coiled-coil pocket of human immunodeficiency virus type 1 gp41 are essential for viral replication and interhelical interaction
Hongmei Mo
, 
, Alex K. Konstantinidis, Kent D. Stewart, Tatyana Dekhtyar, Teresa Ng, Kerry Swift, Edmund D. Matayoshi, Warren Kati, William Kohlbrenner and Akhteruzzaman Molla
Received 29 June 2004;
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Abstract
The human immunodeficiency virus type 1 (HIV-1) gp41 plays an important role in mediating the fusion of HIV with host cells. During the fusion process, three N-terminal helices and three C-terminal helices pack in an anti-parallel direction to form a six-helix bundle. X-ray crystallographic analysis of the gp41 core demonstrated that within each coiled-coil interface, there is a deep and large pocket, formed by a cluster of residues in the N-helix coiled-coil. In this report, we systematically analyzed the role of seven conserved residues that are either lining or packing this pocket on the infectivity and interhelical interaction using novel approaches. Our results show that residues L568, V570, W571, and K574 of the N-helix that are lining the side chain and right wall of the pocket are important for establishing a productive infection. Mutations V570A and W571A completely abolished replication, while replication of the L568A and K574A mutants was significantly attenuated relative to wild type. Similarly, residues W628, W631, and I635 of the C-helix that insert into the pocket are essential for infectivity. The impaired infectivity of these seven mutants is in part attributed to the loss in binding affinity of the interhelical interaction. Molecular modeling of the crystal structure of the coiled-coil further shows that alanine substitution of those residues disrupts the hydrophobic interaction between the N- and C-helix. These results suggest that the conserved residues in the coiled-coil domain play a key role in HIV infection and this coiled-coil pocket is a good target for development of inhibitors against HIV. In addition, our data indicate that the novel fluorescence polarization assay described in this study could be valuable in screening for inhibitors that block the interhelical interaction and HIV entry.
Keywords: Coiled-coil; Viral replication; Interhelical interaction
Article Outline
- Introduction
- Results
- Residues comprising the cavity and inserting into the cavity are essential for viral replication
- Binding assay
- Effect of gp41 mutations on interaction between N- and C-helix
- Inhibition of HIV infection by mutant C-peptides
- Molecular modeling of mutations
- Discussion
- Materials and methods
- Construction of mutants
- Construction and expression of MBP-N-helix for wild-type (WT) and mutants
- Binding assay
- Transfection
- Infectivity assay
- Synthesis of WT and mutant C-peptide
- Peptide inhibition assay
- Molecular modeling
- Acknowledgements
- References
