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本文引用的文献

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Increased breadth of HIV-1 neutralization achieved by diverse antibody clones each with limited neutralization breadth.多种抗体克隆均可提高 HIV-1 中和广度,而每种克隆的中和广度有限。
PLoS One. 2018 Dec 19;13(12):e0209437. doi: 10.1371/journal.pone.0209437. eCollection 2018.
2
B cells with aberrant activation of Notch1 signaling promote Treg and Th2 cell-dominant T-cell responses via IL-33.Notch1 信号异常激活的 B 细胞通过 IL-33 促进 Treg 和 Th2 细胞主导的 T 细胞应答。
Blood Adv. 2018 Sep 25;2(18):2282-2295. doi: 10.1182/bloodadvances.2018019919.
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Correlates of adjuvanticity: A review on adjuvants in licensed vaccines.佐剂的相关性:已上市疫苗中的佐剂概述。
Semin Immunol. 2018 Oct;39:14-21. doi: 10.1016/j.smim.2018.05.001. Epub 2018 May 23.
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Anti-HIV IgM protects against mucosal SHIV transmission.抗 HIV IgM 可预防黏膜 SHIV 传播。
AIDS. 2018 Jul 17;32(11):F5-F13. doi: 10.1097/QAD.0000000000001857.
5
A Highly Potent and Broadly Neutralizing H1 Influenza-Specific Human Monoclonal Antibody.一种高效且广谱中和的 H1 型流感特异性人源单克隆抗体。
Sci Rep. 2018 Mar 12;8(1):4374. doi: 10.1038/s41598-018-22307-8.
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Control of B-1a cell development by instructive BCR signaling.指导型 BCR 信号对 B-1a 细胞发育的控制。
Curr Opin Immunol. 2018 Apr;51:24-31. doi: 10.1016/j.coi.2018.01.001. Epub 2018 Feb 3.
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HIV Infection and AIDS in Sub-Saharan Africa: Current Status, Challenges and Opportunities.撒哈拉以南非洲地区的艾滋病毒感染与艾滋病:现状、挑战与机遇
Open AIDS J. 2016 Apr 8;10:34-48. doi: 10.2174/1874613601610010034. eCollection 2016.
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Achieving Potent Autologous Neutralizing Antibody Responses against Tier 2 HIV-1 Viruses by Strategic Selection of Envelope Immunogens.通过对包膜免疫原进行策略性选择实现针对2级HIV-1病毒的强效自体中和抗体反应。
J Immunol. 2016 Apr 1;196(7):3064-78. doi: 10.4049/jimmunol.1500527. Epub 2016 Mar 4.
9
Recent Developments in Preclinical DNA Vaccination.临床前DNA疫苗接种的最新进展
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10
IL-33 released by alum is responsible for early cytokine production and has adjuvant properties.明矾释放的白细胞介素-33负责早期细胞因子的产生,并具有佐剂特性。
Sci Rep. 2015 Aug 14;5:13146. doi: 10.1038/srep13146.

白细胞介素-33 增强了针对 HIV-1 Env 疫苗的 DNA 和蛋白质的抗体反应的动力学和质量。

IL-33 enhances the kinetics and quality of the antibody response to a DNA and protein-based HIV-1 Env vaccine.

机构信息

Infectious Diseases Division, University of Rochester Medical Center, Rochester, NY, United States.

Department of Microbiology & Immunology, University of Rochester Medical Center, Rochester, NY, United States.

出版信息

Vaccine. 2019 Apr 17;37(17):2322-2330. doi: 10.1016/j.vaccine.2019.03.044. Epub 2019 Mar 27.

DOI:10.1016/j.vaccine.2019.03.044
PMID:30926296
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6506229/
Abstract

Induction of a sustained and broad antibody (Ab) response is a major goal in developing a protective HIV-1 vaccine. DNA priming alone shows reduced levels of immunogenicity; however, when combined with protein boosting is an attractive vaccination strategy for induction of humoral responses. Using the VC10014 DNA and protein-based vaccine consisting of HIV-1 envelope (Env) gp160 plasmids and trimeric gp140 proteins derived from an HIV-1 clade B infected subject who developed broadly neutralizing serum Abs, and which has been previously demonstrated to induce Tier 2 heterologous neutralizing Abs in rhesus macaques, we evaluated whether MPLA and IL-33 when administered during the DNA priming phase enhances the humoral response in mice. The addition of IL-33 during the gp160 DNA priming phase resulted in high titer gp120-specific plasma IgG after the first immunization. The IL-33 treated mice had higher plasma IgG Ab avidity, breadth, and durability after DNA and protein co-immunization with alum adjuvant as compared to MPLA and alum only treated mice. IL-33 was also associated with a significant IgM Env-specific response and expansion of peritoneal and splenic B-1b B cells. These results indicate that DNA priming in the presence of exogenous IL-33 qualitatively alters the HIV-1 Env-specific humoral response, improving the kinetics and breadth of potentially protective Ab.

摘要

诱导持续广泛的抗体(Ab)反应是开发保护性 HIV-1 疫苗的主要目标。单独的 DNA 引发显示出较低的免疫原性;然而,当与蛋白质增强结合使用时,对于诱导体液反应是一种有吸引力的疫苗接种策略。使用由 HIV-1 包膜(Env)gp160 质粒和源自感染 HIV-1 分群 B 的个体的三聚体 gp140 蛋白组成的 VC10014 DNA 和基于蛋白质的疫苗,该个体产生了广泛中和血清 Abs,并且先前已经证明可以在恒河猴中诱导 2 级异源中和 Abs,我们评估了在 DNA 引发阶段给予 MPLA 和 IL-33 是否增强了小鼠中的体液反应。在 gp160 DNA 引发阶段添加 IL-33 后,第一次免疫后会产生高滴度的 gp120 特异性血浆 IgG。与 MPLA 和仅用 alum 处理的小鼠相比,用 IL-33 处理的小鼠在 DNA 和蛋白质与 alum 共同免疫后具有更高的血浆 IgG Ab 亲和力、广度和持久性。IL-33 还与显著的 IgM Env 特异性反应和腹膜和脾脏 B-1b B 细胞的扩增相关。这些结果表明,存在外源性 IL-33 的 DNA 引发从质量上改变了 HIV-1 Env 特异性体液反应,改善了潜在保护性 Ab 的动力学和广度。