Identification of Amino Acids in the Human Tetherin Transmembrane Domain Responsible for HIV-1 Vpu Interaction and Susceptibility

被引:70
作者
Kobayashi, Tomoko [1 ]
Ode, Hirotaka [2 ]
Yoshida, Takeshi [1 ,3 ]
Sato, Kei [1 ]
Gee, Peter [1 ]
Yamamoto, Seiji P. [1 ,4 ]
Ebina, Hirotaka [1 ]
Strebel, Klaus [3 ]
Sato, Hironori [2 ]
Koyanagi, Yoshio [1 ]
机构
[1] Kyoto Univ, Lab Viral Pathogenesis, Inst Virus Res, Sakyo Ku, Kyoto 6068507, Japan
[2] Natl Inst Infect Dis, Pathogen Genom Ctr, Tokyo 2080011, Japan
[3] NIAID, Mol Microbiol Lab, Viral Biochem Sect, NIH, Bethesda, MD 20892 USA
[4] Kyoto Univ, Dept Mol & Cellular Biol, Grad Sch Biostudies, Sakyo Ku, Kyoto 6068507, Japan
基金
日本学术振兴会;
关键词
HUMAN-IMMUNODEFICIENCY-VIRUS; MOLECULAR-DYNAMICS SIMULATIONS; PARTICLE MESH EWALD; AMBER FORCE-FIELD; TYPE-1; VPU; FLUORESCENCE COMPLEMENTATION; PROTEIN INTERACTIONS; MEMBRANE-PROTEIN; CELL-SURFACE; LIVING CELLS;
D O I
10.1128/JVI.01668-10
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
Tetherin, also known as BST-2/CD317/HM1.24, is an antiviral cellular protein that inhibits the release of HIV-1 particles from infected cells. HIV-1 viral protein U (Vpu) is a specific antagonist of human tetherin that might contribute to the high virulence of HIV-1. In this study, we show that three amino acid residues (I34, L37, and L41) in the transmembrane (TM) domain of human tetherin are critical for the interaction with Vpu by using a live cell-based assay. We also found that the conservation of an additional amino acid at position 45 and two residues downstream of position 22, which are absent from monkey tetherins, are required for the antagonism by Vpu. Moreover, computer-assisted structural modeling and mutagenesis studies suggest that an alignment of these four amino acid residues (I34, L37, L41, and T45) on the same helical face in the TM domain is crucial for the Vpu-mediated antagonism of human tetherin. These results contribute to the molecular understanding of human tetherin-specific antagonism by HIV-1 Vpu.
引用
收藏
页码:932 / 945
页数:14
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