Comparative immunogenicity of an mRNA/LNP and a DNA vaccine targeting HIV gag conserved elements in macaques

被引:13
|
作者
Valentin, Antonio [1 ]
Bergamaschi, Cristina [2 ]
Rosati, Margherita [1 ]
Angel, Matthew [3 ,4 ]
Burns, Robert [2 ]
Agarwal, Mahesh [2 ]
Gergen, Janina [5 ]
Petsch, Benjamin [5 ]
Oostvogels, Lidia [5 ]
Loeliger, Edde [5 ]
Chew, Kara W. [6 ]
Deeks, Steven G. [7 ]
Mullins, James I. [8 ,9 ,10 ]
Pavlakis, George N. [1 ]
Felber, Barbara K. [2 ]
机构
[1] Natl Canc Inst Frederick, Ctr Canc Res, Vaccine Branch, Human Retrovirus Sect, Frederick, MD USA
[2] Natl Canc Inst Frederick, Ctr Canc Res, Vaccine Branch, Human Retrovirus Pathogenesis Sect, Frederick, MD 21702 USA
[3] Natl Cncer Inst, Ctr Canc Res, Vaccine Branch, Bethesda, MD USA
[4] Leidos Biomed Res Inc, Frederick Natl Lab Canc Res, Ctr Canc Res Collaborat Bioinformat Resource, Frederick, MD USA
[5] CureVac AG, Tubingen, Germany
[6] Univ Calif Los Angeles, Dept Med, David Geffen Sch Med, Los Angeles, CA USA
[7] Univ Calif San Francisco, Div HIV Infect Dis & Global Med, San Francisco, CA USA
[8] Univ Washington, Dept Microbiol, Seattle, WA USA
[9] Univ Washington, Dept Med, Seattle, WA USA
[10] Univ Washington, Dept Global Hlth, Seattle, WA USA
来源
FRONTIERS IN IMMUNOLOGY | 2022年 / 13卷
基金
美国国家卫生研究院;
关键词
mRNA; LNP; therapeutic immunization; HIV; T cell response; antibody; gag; conserved sequences; immune focusing; CELLULAR IMMUNE-RESPONSES; SIMIAN IMMUNODEFICIENCY VIRUS; MESSENGER-RNA VACCINES; YELLOW-FEVER VACCINE; T-CELLS; SYSTEMS BIOLOGY; MOSAIC VACCINE; EPITOPES; BREADTH; IL-17;
D O I
10.3389/fimmu.2022.945706
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Immunogenicity of HIV-1 mRNA vaccine regimens was analyzed in a non-human primate animal model. Rhesus macaques immunized with mRNA in lipid nanoparticle (mRNA/LNP) formulation expressing HIV-1 Gag and Gag conserved regions (CE) as immunogens developed robust, durable antibody responses but low adaptive T-cell responses. Augmentation of the dose resulted in modest increases in vaccine-induced cellular immunity, with no difference in humoral responses. The gag mRNA/lipid nanoparticle (LNP) vaccine provided suboptimal priming of T cell responses for a heterologous DNA booster vaccination regimen. In contrast, a single immunization with gag mRNA/LNP efficiently boosted both humoral and cellular responses in macaques previously primed by a gag DNA-based vaccine. These anamnestic cellular responses were mediated by activated CD8(+) T cells with a phenotype of differentiated T-bet(+) cytotoxic memory T lymphocytes. The heterologous prime/boost regimens combining DNA and mRNA/LNP vaccine modalities maximized vaccine-induced cellular and humoral immune responses. Analysis of cytokine responses revealed a transient systemic signature characterized by the release of type I interferon, IL-15 and IFN-related chemokines. The pro-inflammatory status induced by the mRNA/LNP vaccine was also characterized by IL-23 and IL-6, concomitant with the release of IL-17 family of cytokines. Overall, the strong boost of cellular and humoral immunity induced by the mRNA/LNP vaccine suggests that it could be useful as a prophylactic vaccine in heterologous prime/boost modality and in immune therapeutic interventions against HIV infection or other chronic human diseases.
引用
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页数:17
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