Vaccine with bacterium-like particles displaying HIV-1 gp120 trimer elicits specific mucosal responses and neutralizing antibodies in rhesus macaques

IF 4.8 2区 生物学 Q1 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Microbial Biotechnology Pub Date : 2022-03-15 DOI:10.1111/1751-7915.14022
Huaiyu Wang, Pingchao Li, Mo Zhang, Jinpeng Bi, Yizi He, Fangshen Li, Rongzhen Yu, Feng Gao, Wei Kong, Bin Yu, Ling Chen, Xianghui Yu
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引用次数: 3

Abstract

Preclinical studies have shown that the induction of secretory IgA (sIgA) in mucosa and neutralizing antibodies (NAbs) in sera is essential for designing vaccines that can effectively block the transmission of HIV-1. We previously showed that a vaccine consisting of bacterium-like particles (BLPs) displaying Protan-gp120AE-MTQ (PAM) could induce mucosal immune responses through intranasal (IN) immunization in mice and NAbs through intramuscular (IM) immunization in guinea pigs. Here, we evaluated the ability of this vaccine BLP-PAM to elicit HIV-1-specific mucosal and systemic immune responses through IN and IM immunization combination strategies in rhesus macaques. First, the morphology, antigenicity and epitope accessibility of the vaccine were analysed by transmission electron microscopy, bio-layer interferometry and ELISA. In BLP-PAM-immunized macaques, HIV-1-specific sIgA were rapidly induced through IN immunization in situ and distant mucosal sites, although the immune responses are relatively weak. Furthermore, the HIV-1-specific IgG and IgA antibody levels in mucosal secretions were enhanced and maintained, while production of serum NAbs against heterologous HIV-1 tier 1 and 2 pseudoviruses was elicited after IM boost. Additionally, situ mucosal responses and systemic T cell immune responses were improved by rAd2-gp120AE boost immunization via the IN and IM routes. These results suggested that BLP-based delivery in combination with the IN and IM immunization approach represents a potential vaccine strategy against HIV-1.

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显示HIV-1 gp120三聚体的细菌样颗粒疫苗在恒河猴中引起特异性粘膜反应和中和抗体
临床前研究表明,诱导粘膜分泌IgA (sIgA)和血清中和抗体(nab)对于设计有效阻断HIV-1传播的疫苗至关重要。我们之前的研究表明,一种由显示Protan-gp120AE-MTQ (PAM)的细菌样颗粒(BLPs)组成的疫苗可以通过小鼠鼻内(IN)免疫诱导粘膜免疫反应,并通过豚鼠肌内(IM)免疫诱导nab。在这里,我们评估了该疫苗BLP-PAM通过IN和IM联合免疫策略在恒河猴中引发hiv -1特异性粘膜和全身免疫反应的能力。首先,采用透射电镜、生物层干涉法和酶联免疫吸附法对疫苗的形态、抗原性和表位可及性进行分析。在blp - pam免疫的猕猴中,尽管免疫反应相对较弱,但通过原位和远处粘膜部位的In免疫可以快速诱导hiv -1特异性sIgA。此外,粘膜分泌物中HIV-1特异性IgG和IgA抗体水平得到增强和维持,而IM增强后可诱导血清中产生针对异源HIV-1 1级和2级假病毒的抗体。此外,通过IN和IM途径增强rAd2-gp120AE免疫可改善原位粘膜反应和全身T细胞免疫反应。这些结果表明,基于blp的递送结合in和IM免疫方法代表了一种潜在的针对HIV-1的疫苗策略。
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来源期刊
Microbial Biotechnology
Microbial Biotechnology BIOTECHNOLOGY & APPLIED MICROBIOLOGY-MICROBIOLOGY
CiteScore
9.80
自引率
3.50%
发文量
162
审稿时长
6-12 weeks
期刊介绍: Microbial Biotechnology publishes papers of original research reporting significant advances in any aspect of microbial applications, including, but not limited to biotechnologies related to: Green chemistry; Primary metabolites; Food, beverages and supplements; Secondary metabolites and natural products; Pharmaceuticals; Diagnostics; Agriculture; Bioenergy; Biomining, including oil recovery and processing; Bioremediation; Biopolymers, biomaterials; Bionanotechnology; Biosurfactants and bioemulsifiers; Compatible solutes and bioprotectants; Biosensors, monitoring systems, quantitative microbial risk assessment; Technology development; Protein engineering; Functional genomics; Metabolic engineering; Metabolic design; Systems analysis, modelling; Process engineering; Biologically-based analytical methods; Microbially-based strategies in public health; Microbially-based strategies to influence global processes
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