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本文引用的文献

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Fc receptor-mediated immune responses: new tools but increased complexity in HIV prevention.Fc受体介导的免疫反应:新工具,但在HIV预防中增加了复杂性。
Curr HIV Res. 2013 Jul;11(5):407-20. doi: 10.2174/1570162x113116660063.
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New paradigms for functional HIV-specific nonneutralizing antibodies.功能性 HIV 特异性非中和抗体的新范例。
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Comparison of intradermal and intramuscular delivery followed by in vivo electroporation of SIV Env DNA in macaques.比较皮内和肌内递送,然后对恒河猴进行 SIV Env DNA 的体内电穿孔。
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Response to the AIDS pandemic--a global health model.应对艾滋病大流行——一种全球健康模式。
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Vaccine-induced plasma IgA specific for the C1 region of the HIV-1 envelope blocks binding and effector function of IgG.疫苗诱导的针对 HIV-1 包膜 C1 区的血浆 IgA 可阻断 IgG 的结合和效应功能。
Proc Natl Acad Sci U S A. 2013 May 28;110(22):9019-24. doi: 10.1073/pnas.1301456110. Epub 2013 May 9.
8
HIV/SIV DNA vaccine combined with protein in a co-immunization protocol elicits highest humoral responses to envelope in mice and macaques.HIV/SIV DNA 疫苗与蛋白质联合使用的共免疫方案可在小鼠和猕猴中引发针对包膜的最高体液免疫反应。
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HIV-1 p24(gag) derived conserved element DNA vaccine increases the breadth of immune response in mice.HIV-1 p24(gag) 衍生保守元件 DNA 疫苗增强了小鼠的免疫反应广度。
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10
Impact of antibody quality and anamnestic response on viremia control post-challenge in a combined Tat/Env vaccine regimen in rhesus macaques.在恒河猴中,联合 Tat/Env 疫苗方案中抗体质量和记忆应答对挑战后病毒血症控制的影响。
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黏膜和/或全身 SIV 特异性疫苗平台诱导的体液免疫提示了增强反应的新的组合方法。

Humoral immunity induced by mucosal and/or systemic SIV-specific vaccine platforms suggests novel combinatorial approaches for enhancing responses.

机构信息

Immune Biology of Retroviral Infection Section, Vaccine Branch, CCR, NCI, NIH, Bethesda, MD 20892, United States.

Animal Models and Retroviral Vaccine Section, Vaccine Branch, CCR, NCI, NIH, Bethesda, MD 20892, United States.

出版信息

Clin Immunol. 2014 Aug;153(2):308-22. doi: 10.1016/j.clim.2014.05.008. Epub 2014 Jun 4.

DOI:10.1016/j.clim.2014.05.008
PMID:24907411
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4102324/
Abstract

Combinatorial HIV/SIV vaccine approaches targeting multiple arms of the immune system might improve protective efficacy. We compared SIV-specific humoral immunity induced in rhesus macaques by five vaccine regimens. Systemic regimens included ALVAC-SIVenv priming and Env boosting (ALVAC/Env); DNA immunization; and DNA plus Env co-immunization (DNA&Env). RepAd/Env combined mucosal replication-competent Ad-env priming with systemic Env boosting. A Peptide/Env regimen, given solely intrarectally, included HIV/SIV peptides followed by MVA-env and Env boosts. Serum antibodies mediating neutralizing, phagocytic and ADCC activities were induced by ALVAC/Env, RepAd/Env and DNA&Env vaccines. Memory B cells and plasma cells were maintained in the bone marrow. RepAd/Env vaccination induced early SIV-specific IgA in rectal secretions before Env boosting, although mucosal IgA and IgG responses were readily detected at necropsy in ALVAC/Env, RepAd/Env, DNA&Env and DNA vaccinated animals. Our results suggest that combined RepAd priming with ALVAC/Env or DNA&Env regimen boosting might induce potent, functional, long-lasting systemic and mucosal SIV-specific antibodies.

摘要

联合 HIV/SIV 疫苗方法靶向免疫系统的多个分支可能会提高保护效力。我们比较了五种疫苗方案在恒河猴中诱导的 SIV 特异性体液免疫。全身方案包括 ALVAC-SIVenv 启动和Env 加强(ALVAC/Env);DNA 免疫;以及 DNA 加 Env 共同免疫(DNA&Env)。RepAd/Env 结合粘膜复制有效的 Ad-env 启动和全身 Env 加强。Peptide/Env 方案仅直肠内给药,包括 HIV/SIV 肽,随后是 MVA-env 和 Env 加强。中和、吞噬和 ADCC 活性介导的血清抗体由 ALVAC/Env、RepAd/Env 和 DNA&Env 疫苗诱导。记忆 B 细胞和浆细胞在骨髓中维持。RepAd/Env 疫苗接种在 Env 加强之前诱导早期直肠分泌物中的 SIV 特异性 IgA,尽管在尸检时在 ALVAC/Env、RepAd/Env、DNA&Env 和 DNA 接种动物中很容易检测到粘膜 IgA 和 IgG 反应。我们的结果表明,结合 RepAd 启动和 ALVAC/Env 或 DNA&Env 方案加强可能会诱导强大、功能、持久的全身和粘膜 SIV 特异性抗体。