The HIV-1 gp120 V1V2 loop: structure, function and importance for vaccine development
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作者:
O'Connell, Robert J.
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Armed Forces Res Inst Med Sci, Bangkok 10400, ThailandArmed Forces Res Inst Med Sci, Bangkok 10400, Thailand
O'Connell, Robert J.
[1
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Kim, Jerome H.
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US Mil HIV Res Program MHRP, Bethesda, MD 20817 USAArmed Forces Res Inst Med Sci, Bangkok 10400, Thailand
Kim, Jerome H.
[2
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Excler, Jean-Louis
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US Mil HIV Res Program MHRP, Bethesda, MD 20817 USA
Henry M Jackson Fdn Adv Mil Med, Bethesda, MD 20817 USAArmed Forces Res Inst Med Sci, Bangkok 10400, Thailand
Excler, Jean-Louis
[2
,3
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机构:
[1] Armed Forces Res Inst Med Sci, Bangkok 10400, Thailand
[2] US Mil HIV Res Program MHRP, Bethesda, MD 20817 USA
[3] Henry M Jackson Fdn Adv Mil Med, Bethesda, MD 20817 USA
Although the second variable loop (V2) of the HIV-1 gp120 envelope glycoprotein shows substantial sequence diversity between strains, its functional importance imposes critical conservation of structure, and within particular microdomains, of sequence. V2 influences HIV-1 viral entry by contributing to trimer stabilization and co-receptor binding. It is one of 4 key domains targeted by the broadly neutralizing antibodies that arise during HIV-1 infection. HIV-1 uses V1V2 sequence variation and glycosylation to escape neutralizing antibody. In the Thai Phase III HIV-1 vaccine trial, RV144, vaccine-induced IgG against V1V2 inversely correlated with the risk of HIV-1 acquisition, and HIV-1 strains infecting RV144 vaccine recipients differed from those infecting placebo recipients in the V2 domain. Similarly, non-human primate challenge studies demonstrated an inverse correlation between vaccine-induced anti-V2 responses and simian immunodeficiency virus acquisition. We hypothesize that increased magnitude, frequency and duration of vaccine-induced anti-V2 antibody responses should improve efficacy afforded by pox-protein prime-boost HIV vaccine strategies.
机构:
Natl Inst Infect Dis, Lab Viral Genom, Pathogen Genom Ctr, Musashimurayama, Tokyo, JapanNatl Inst Infect Dis, Lab Viral Genom, Pathogen Genom Ctr, Musashimurayama, Tokyo, Japan
Yokoyama, Masaru
Naganawa, Satoshi
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Tokyo Metropolitan Inst Med Sci, Dept Microbiol & Cell Biol, Setagaya Ku, Tokyo 113, JapanNatl Inst Infect Dis, Lab Viral Genom, Pathogen Genom Ctr, Musashimurayama, Tokyo, Japan
Naganawa, Satoshi
Yoshimura, Kazuhisa
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Kumamoto Univ, Ctr AIDS Res, Div Clin Retrovirol & Infect Dis, Kumamoto, JapanNatl Inst Infect Dis, Lab Viral Genom, Pathogen Genom Ctr, Musashimurayama, Tokyo, Japan
Yoshimura, Kazuhisa
Matsushita, Shuzo
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Kumamoto Univ, Ctr AIDS Res, Div Clin Retrovirol & Infect Dis, Kumamoto, JapanNatl Inst Infect Dis, Lab Viral Genom, Pathogen Genom Ctr, Musashimurayama, Tokyo, Japan
Matsushita, Shuzo
Sato, Hironori
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Natl Inst Infect Dis, Lab Viral Genom, Pathogen Genom Ctr, Musashimurayama, Tokyo, JapanNatl Inst Infect Dis, Lab Viral Genom, Pathogen Genom Ctr, Musashimurayama, Tokyo, Japan
机构:
Walter Reed Army Inst Res, US Mil HIV Res Program, 503 Robert Grant Ave, Silver Spring, MD 20910 USA
Henry M Jackson Fdn Adv Mil Med, 6720A Rockledge Dr, Bethesda, MD 20817 USAWalter Reed Army Inst Res, US Mil HIV Res Program, 503 Robert Grant Ave, Silver Spring, MD 20910 USA
Karch, Christopher P.
Matyas, Gary R.
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Walter Reed Army Inst Res, US Mil HIV Res Program, 503 Robert Grant Ave, Silver Spring, MD 20910 USAWalter Reed Army Inst Res, US Mil HIV Res Program, 503 Robert Grant Ave, Silver Spring, MD 20910 USA
Matyas, Gary R.
Burkhard, Peter
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Alpha O Peptides, Lorracherstr 50, CH-4125 Riehen, SwitzerlandWalter Reed Army Inst Res, US Mil HIV Res Program, 503 Robert Grant Ave, Silver Spring, MD 20910 USA
Burkhard, Peter
Beck, Zoltan
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Walter Reed Army Inst Res, US Mil HIV Res Program, 503 Robert Grant Ave, Silver Spring, MD 20910 USA
Henry M Jackson Fdn Adv Mil Med, 6720A Rockledge Dr, Bethesda, MD 20817 USAWalter Reed Army Inst Res, US Mil HIV Res Program, 503 Robert Grant Ave, Silver Spring, MD 20910 USA