A novel adjuvant for mucosal immunity to HIV-1 gp120 in nonhuman primates

被引：25

作者：

Yoshino, N

Lü, FXS

Fujihashi, K

Hagiwara, Y

Kataoka, K

Lu, D

Hirst, L

Honda, M

van Ginkel, FW

Takeda, Y

Miller, CJ

Kiyono, H

McGhee, JR

机构：

[1] Univ Alabama Birmingham, Sch Dent, Dept Oral Biol, Immunobiol Vaccine Ctr, Birmingham, AL 35294 USA

[2] Univ Alabama Birmingham, Immunobiol Vaccine Ctr, Dept Microbiol, Birmingham, AL 35294 USA

[3] Univ Calif Davis, Sch Med, Dept Pathol, Calif Reg Primate Res Ctr, Davis, CA 95616 USA

[4] Univ Tokyo, Inst Med Sci, Dept Microbiol & Immunol, Div Mucosal Immunol, Tokyo, Japan

来源：

JOURNAL OF IMMUNOLOGY | 2004年 / 173卷 / 11期

关键词：

D O I：

10.4049/jimmunol.173.11.6850

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

The development of a safe and effective mucosal adjuvant is a crucial step toward a mucosal HIV/AIDS vaccine. This study seeks to determine the promise of a nontoxic mutant of cholera toxin (mCT; E112K) as a mucosal adjuvant in nonhuman primates. HIV-1 gp120 was nasally administered together with mCT E112K or native CT (nCT) as adjuvant on five to six occasions over a 6- to 8-wk period to groups of four rhesus macaques and alone to two monkeys that acted as controls. Macaques given nasal gp120 with either mCT E112K or nCT showed elevated gp120-specific IgG and IgA Ab responses with virus-neutralizing activity in both their plasma and mucosal external secretions, as well as higher numbers of gp120-specific IgA Ab-forming cells in their mucosal and peripheral lymphoid tissues and of IL-4-producing Th2-type CD4-positive (CD4(+)) T cells than did controls. Even though significant mucosal adjuvanticity was seen with both mCT E112K and nCT, neuronal damage was observed only in the nCT-treated, but not in the control or mCT E112K-treated groups. These results clearly show that mCT E112K is an effective and safe mucosal adjuvant for the development of a nasal HIV/AIDS vaccine.

引用

页码：6850 / 6857

页数：8

共 50 条

[21] Intracellular signalling mediating HIV-1 gp120 neurotoxicity
Scorziello, A
Florio, T
Bajetto, A
Schettini, G
CELLULAR SIGNALLING, 1998, 10 (02) : 75 - 84
[22] Molecular architecture of native HIV-1 gp120 trimers
Liu, Jun
Bartesaghi, Alberto
Borgnia, Mario J.
Sapiro, Guillermo
Subramaniam, Sriram
NATURE, 2008, 455 (7209) : 109 - U76
[23] DIFFERENTIAL-EFFECTS OF HIV-1 GP120 ON THYMOCYTES
OYAIZU, N
CHIRMULE, N
YAGURA, H
SUGIURA, K
MCCLOSKEY, T
KALYANARAMAN, VS
PAHWA, S
FASEB JOURNAL, 1992, 6 (05): : A1978 - A1978
[24] Molecular architecture of native HIV-1 gp120 trimers
Jun Liu
Alberto Bartesaghi
Mario J. Borgnia
Guillermo Sapiro
Sriram Subramaniam
Nature, 2008, 455 : 109 - 113
[25] CHARACTERISTICS OF HIV-1 GP120 GLYCOPROTEIN BINDING TO GLYCOLIPIDS
MCALARNEY, T
APOSTOLSKI, S
LEDERMAN, S
LATOV, N
JOURNAL OF NEUROSCIENCE RESEARCH, 1994, 37 (04) : 453 - 460
[26] Inhibitory effects of HIV-1 gp120 on myelin formation
KimuraKuroda, J
Nagashima, K
Yasui, K
PERSPECTIVES IN DRUG DISCOVERY AND DESIGN, 1996, 5 : 17 - 29
[27] Search for nearly invariant segments in HIV-1 gp120
Wu, TT
Johnson, G
BIOPHYSICAL JOURNAL, 2003, 84 (02) : 282A - 282A
[28] Structural flexibility and rigidity analysis of HIV-1 gp120
Tan, Hepan
Rader, A. J.
JOURNAL OF BIOMOLECULAR STRUCTURE & DYNAMICS, 2007, 24 (06): : 768 - 769
[29] SEVERAL ANTIGENIC DETERMINANTS EXPOSED ON THE GP120 MOIETY OF HIV-1 GP160 ARE HIDDEN ON THE MATURE GP120
THIRIART, C
FRANCOTTE, M
COHEN, J
COLLIGNON, C
DELERS, A
KUMMERT, S
MOLITOR, C
GILLES, D
ROELANTS, P
VANWIJNENDAELE, F
DEWILDE, M
BRUCK, C
JOURNAL OF IMMUNOLOGY, 1989, 143 (06): : 1832 - 1836
[30] INVITRO INHIBITION OF IMMUNE FUNCTIONS BY GP120 OF HIV-1
SIRIANNI, MC
PONTESILLI, O
DELUCA, S
TAGLIAFERRI, F
LOVIGO, C
CARLESIMO, M
VARANI, AR
AIUTI, F
AIDS RESEARCH AND HUMAN RETROVIRUSES, 1991, 7 (02) : 139 - 140

← 1 2 3 4 5 →