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表达猿猴免疫缺陷病毒包膜的二价嵌合狂犬病病毒诱导多功能抗体反应。

A Bivalent, Chimeric Rabies Virus Expressing Simian Immunodeficiency Virus Envelope Induces Multifunctional Antibody Responses.

作者信息

Dunkel Amber, Shen Shixue, LaBranche Celia C, Montefiori David, McGettigan James P

机构信息

1 Department of Microbiology and Immunology, Thomas Jefferson University , Philadelphia, Pennsylvania.

2 Department of Surgery, Duke University , Durham, North Carolina.

出版信息

AIDS Res Hum Retroviruses. 2015 Nov;31(11):1126-38. doi: 10.1089/AID.2014.0319. Epub 2015 May 5.

Abstract

We previously showed that a matrix (M) gene-deleted rabies virus (RABV)-based vaccine (RABV-ΔM) is highly immunogenic and induces potent B cell responses in the context of RABV infection. We speculated that RABV-ΔM expressing HIV proteins would also induce potent B cell responses against HIV antigens. As a prerequisite to future studies in nonhuman primates, we completed immunogenicity studies in mice to confirm the ability of RABV-ΔM to induce polyfunctional B cell responses in the context of HIV. To that end, the envelope protein from the mac239 strain of SIV (SIVmac239Env) was cloned into RABV-ΔM, resulting in RABV-ΔM-Env. Infectious virus was recovered following standard methods and propagated on baby hamster kidney cells stably expressing RABV M [>10(7) focus forming units (ffu)/ml]. Western blot analysis of cell lysates or of purified virions confirmed Env expression on the surface of infected cells and within virus particles, respectively. Positive neutralization activity against a neutralization-sensitive SIV strain and to a lesser extent against a neutralization-resistant SIV strain was detected in mice after a single intramuscular inoculation with RABV-ΔM-Env. The quality, but not quantity, of the antibody response was enhanced via boosting with recombinant gp130 or RABV-ΔM-Env as measured by an increase in antibody avidity and a skewing toward a Th1-type antibody response. We also show that an intradermal inoculation induces higher antibodies than an intramuscular or intranasal inoculation. An intradermal inoculation of RABV-ΔM-Env followed by a boost inoculation with recombinant gp130 produced anti-SIV antibodies with neutralizing and nonneutralizing antibody (nNAb) effector functions. Together, RABV-ΔM-Env induces B cells to secrete antibodies against SIV with the potential to clear both "free" and cell-associated virus. Strategies capable of eliciting both NAbs as well as nNAbs might help to improve the efficacy of HIV-1 vaccines.

摘要

我们之前表明,一种基于基质(M)基因缺失的狂犬病病毒(RABV)的疫苗(RABV-ΔM)具有高度免疫原性,并在RABV感染的情况下诱导强烈的B细胞反应。我们推测,表达HIV蛋白的RABV-ΔM也会诱导针对HIV抗原的强烈B细胞反应。作为未来在非人类灵长类动物中进行研究的前提条件,我们在小鼠中完成了免疫原性研究,以确认RABV-ΔM在HIV背景下诱导多功能B细胞反应的能力。为此,将来自SIV mac239毒株的包膜蛋白(SIVmac239Env)克隆到RABV-ΔM中,得到RABV-ΔM-Env。按照标准方法回收感染性病毒,并在稳定表达RABV M的幼仓鼠肾细胞上进行传代培养[>10(7)蚀斑形成单位(ffu)/毫升]。对细胞裂解物或纯化病毒粒子进行的蛋白质印迹分析分别证实了Env在感染细胞表面和病毒颗粒内的表达。在小鼠单次肌肉注射RABV-ΔM-Env后,检测到针对一种中和敏感的SIV毒株以及在较小程度上针对一种中和抗性的SIV毒株的阳性中和活性。通过用重组gp130或RABV-ΔM-Env加强免疫,抗体亲和力增加且倾向于Th1型抗体反应,从而提高了抗体反应的质量而非数量。我们还表明,皮内接种诱导产生的抗体比肌肉注射或鼻内接种更多。皮内接种RABV-ΔM-Env后再用重组gp130加强免疫,产生了具有中和和非中和抗体(nNAb)效应功能的抗SIV抗体。总之,RABV-ΔM-Env诱导B细胞分泌针对SIV的抗体,有可能清除“游离”和细胞相关病毒。能够引发中和抗体以及非中和抗体的策略可能有助于提高HIV-1疫苗的效力。

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