Immunogenicity of synthetic HIV-1 V3 loop peptides by MPL adjuvanted pH-sensitive liposomes

被引：25

作者：

Chang, JS ^{[1
]}

Choi, MJ ^{[1
]}

Kim, TY ^{[1
]}

Cho, SY ^{[1
]}

Cheong, HS ^{[1
]}

机构：

[1] Mogam Biotechnol Res Inst, Drug Delivery Res Lab, Yongin City 449910, Kyonggi Do, South Korea

来源：

VACCINE | 1999年 / 17卷 / 11-12期

关键词：

pH-sensitive liposomes; cytotoxic T-lymphocytes; neutralizing antibody; V3 loop peptide; HIV vaccine;

D O I：

10.1016/S0264-410X(98)00353-3

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

A successful HIV-1 vaccine should be capable of generating humoral and cellular immune responses at the same rime. The only response shown to be effective in this regard is virus-neutralization antibodies and virus-specific cytotoxic T-lymphocytes (CTL) directed against the viral antigens. In the present study, it is shown that V3 peptides encapsulated pH-sensitive liposomes elicit the virus neutralization antibodies and virus specific CTL response at the same time in Balb/c mice. None of the immunization protocols elicited an antibody response and CTL response when R15K and T26K was used as immunogen without liposomes. In contrast, antibodies and CTL response were detectable in the mice which were immunized with peptide encapsulated pH-sensitive liposomes. Antibody production was confirmed by virus neutralizing assay. CD4+ T-cells are involved in target cell lysis to some degree but CTL activity is mainly due to the CD8+ T-cells. The consistency of the antibody and CTL response was related to the V3 loop peptides size. The T26K (26mer) peptide induced a stronger antibody and CTL response than R15K (15mer) in vivo. Based on the results of this study, T26K was used as a potentially effective HIV-1 vaccine component and T26K encapsulated pi-I-sensitive liposomes composed of phosphatidylethanolaminl-beta-oleoyl-gamma-palmitoyl (POPE)/cholesterol hemisuccinate (CHOH)/monophosphoryl lipid A (MPL) (7:3:0.1, mole ratio) may be used as a potentially immunomodulating adjuvant system for the development of HIV and other viral vaccines. (C) 1999 Elsevier Science Ltd. All rights reserved.

引用

页码：1540 / 1548

页数：9

共 31 条

[1] ENVELOPE PROTEIN AND P18(IIIB) PEPTIDE RECOGNIZED BY CYTOTOXIC T-LYMPHOCYTES FROM HUMANS IMMUNIZED WITH HUMAN-IMMUNODEFICIENCY-VIRUS ENVELOPE
ACHOUR, A
PICARD, O
MBIKA, JP
WILLER, A
SNART, R
BIZZINI, B
CARELLI, C
BURNY, A
ZAGURY, D
[J]. VACCINE, 1993, 11 (07) : 699 - 701
[2] CYTOTOXIC T-LYMPHOCYTES SPECIFIC FOR HIV-1 GP160 ANTIGEN AND SYNTHETIC P18III(B) PEPTIDE IN AN HLA-A11-IMMUNIZED INDIVIDUAL
ACHOUR, A
LEMHAMMEDI, S
PICARD, O
MBIKA, JP
ZAGURY, JF
MOUKRIM, Z
WILLER, A
BEIX, F
BURNY, A
ZAGURY, D
[J]. AIDS RESEARCH AND HUMAN RETROVIRUSES, 1994, 10 (01) : 19 - 25
[3] Molecular analysis of presentation by HLA-A2.1 of a promiscuously binding V3 loop peptide from the HIV-1 envelope protein to human cytotoxic T lymphocytes
AlexanderMiller, MA
Parker, KC
Tsukui, T
Pendleton, CD
Coligan, JE
Berzofsky, JA
[J]. INTERNATIONAL IMMUNOLOGY, 1996, 8 (05) : 641 - 649
[4] LIPOSOMES AS CARRIERS OF ANTIGENS AND ADJUVANTS
ALVING, CR
[J]. JOURNAL OF IMMUNOLOGICAL METHODS, 1991, 140 (01) : 1 - 13
[5] ALVING CR, 1993, J LIPOSOME RES, V3, P493
[6] BEROZOFSKY JA, 1991, FASEB J, V5, P2412
[7] CROSS-REACTIVE CYTOTOXIC T-LYMPHOCYTES INDUCED BY V3 LOOP SYNTHETIC PEPTIDES FROM DIFFERENT STRAINS OF HUMAN-IMMUNODEFICIENCY-VIRUS TYPE-1
CASEMENT, KS
NEHETE, PN
ARLINGHAUS, RB
SASTRY, KJ
[J]. VIROLOGY, 1995, 211 (01) : 261 - 267
[8] PH-SENSITIVE LIPOSOMES CONTAINING POLYMERIZED PHOSPHATIDYLETHANOLAMINE AND FATTY-ACID
CHOI, MJ
HAN, HS
KIM, HM
[J]. JOURNAL OF BIOCHEMISTRY, 1992, 112 (05) : 694 - 699
[9] NEUTRALIZATION OF DIVERSE HUMAN-IMMUNODEFICIENCY-VIRUS TYPE-1 VARIANTS BY AN ANTI-V3 HUMAN MONOCLONAL-ANTIBODY
GORNY, MK
CONLEY, AJ
KARWOWSKA, S
BUCHBINDER, A
XU, JY
EMINI, EA
KOENIG, S
ZOLLAPAZNER, S
[J]. JOURNAL OF VIROLOGY, 1992, 66 (12) : 7538 - 7542
[10] LIPOSOMES AS IMMUNOLOGICAL ADJUVANTS - ANTIGEN INCORPORATION STUDIES
GREGORIADIS, G
DAVIS, D
DAVIES, A
[J]. VACCINE, 1987, 5 (02) : 145 - 151

← 1 2 3 4 →