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白细胞介素-7 佐剂阴道疫苗在非人灵长类动物中引发强烈的黏膜免疫应答。

IL-7-Adjuvanted Vaginal Vaccine Elicits Strong Mucosal Immune Responses in Non-Human Primates.

机构信息

Laboratory of Dendritic Cells, B Lymphocytes and Cytokines in their Microenvironment During Viral Infections and Cancer, Department of Infection, Immunity and Inflammation, Université de Paris, INSERM, CNRS, Institut Cochin, Paris, France.

Laboratory of Mucosal Entry of HIV-1 and Mucosal Immunity, Department of Infection, Immunity and Inflammation, Université de Paris, INSERM, CNRS, Institut Cochin, Paris, France.

出版信息

Front Immunol. 2021 Feb 25;12:614115. doi: 10.3389/fimmu.2021.614115. eCollection 2021.

Abstract

Mucosal immune responses are crucial in protecting against pathogens entering through mucosal surfaces. However, due to poor T-cell responsiveness upon mucosal antigenic stimulation, mucosal immunity remains difficult to obtain through vaccines and requires appropriate adjuvants. We previously demonstrated that administered systemically to healthy macaques or locally expressed in the intestinal mucosa of acutely SIV-infected macaques, interleukin-7 (IL-7) triggers chemokine expression and immune cell homing into mucosae, suggesting its important role in the development of mucosal immune responses. We therefore examined whether local delivery of recombinant glycosylated simian IL-7 (rs-IL-7gly) to the vaginal mucosa of rhesus macaques could prepare the lower female genital tract (FGT) for subsequent immunization and act as an efficient mucosal adjuvant. First, we showed that local administration of rs-IL-7gly triggers vaginal overexpression of chemokines and infiltration of mDCs, macrophages, NKs, B- and T-cells in the lamina propria while MamuLa-DR APCs accumulated in the epithelium. Subsequent mucosal anti-DT immunization in macaques resulted in a faster, stronger, and more persistent mucosal antibody response compared to DT-immunization alone. Indeed, we detected robust productions of DT-specific IgAs and IgGs in their vaginal secretions and identified cells secreting DT-specific IgAs in their vaginal mucosa and IgGs in draining lymph nodes. Finally, the expression of chemokines involved in the organization of tertiary lymphoid structures (TLS) was only increased in the vaginal mucosa of IL-7-adjuvanted immunized macaques. Interestingly, TLSs developed around PNAd high endothelial venules in their lower FGT sampled 2 weeks after the last immunization. Non-traumatic vaginal administration of rs-IL-7gly prepares the mucosa to respond to subsequent local immunization and allows the development of a strong mucosal immune response in macaques, through the chemokine-dependent recruitment of immune cells, the activation of mDCs and the formation of TLSs. The localization of DT-specific IgA plasma cells in the upper vaginal mucosa argues for their contribution to the production of specific immunoglobulins in the vaginal secretions. Our results highlight the potential of IL-7 as a potent mucosal adjuvant to stimulate the FGT immune system and elicit vaginal antibody responses to local immunization, which is the most promising way to confer protection against many sexually transmitted diseases.

摘要

黏膜免疫反应对于防止病原体通过黏膜表面进入至关重要。然而,由于黏膜抗原刺激时 T 细胞反应不佳,因此仍然难以通过疫苗获得黏膜免疫,需要适当的佐剂。我们之前的研究表明,白细胞介素 7(IL-7)全身性给予健康猕猴或局部表达于急性 SIV 感染猕猴的肠道黏膜,可触发趋化因子表达和免疫细胞归巢至黏膜,提示其在黏膜免疫反应的发展中具有重要作用。因此,我们研究了将重组糖基化的猴 IL-7(rs-IL-7gly)局部递送至恒河猴的阴道黏膜是否可以使下生殖道(FGT)为随后的免疫接种做好准备,并作为有效的黏膜佐剂。首先,我们表明,rs-IL-7gly 的局部给药会引发阴道中趋化因子的过度表达和 mDC、巨噬细胞、NK、B 和 T 细胞在固有层中的浸润,而 MamuLa-DR APC 则聚集在上皮中。随后在猕猴中进行黏膜抗 DT 免疫接种会导致与单独 DT 免疫接种相比更快、更强和更持久的黏膜抗体反应。事实上,我们在阴道分泌物中检测到了大量的 DT 特异性 IgA 和 IgG,并在阴道黏膜中鉴定出分泌 DT 特异性 IgA 的细胞和引流淋巴结中的 IgG。最后,只有在 IL-7 佐剂免疫接种的猕猴的阴道黏膜中,参与三级淋巴结构(TLS)形成的趋化因子的表达才会增加。有趣的是,在最后一次免疫接种后 2 周,在下生殖道取样时,在 PNAd 高内皮静脉周围形成了 TLS。rs-IL-7gly 的非创伤性阴道给药可使黏膜对随后的局部免疫接种做出反应,并通过趋化因子依赖的免疫细胞募集、mDC 的激活和 TLS 的形成,在猕猴中引发强烈的黏膜免疫反应。DT 特异性 IgA 浆细胞在上阴道黏膜中的定位表明它们有助于阴道分泌物中特异性免疫球蛋白的产生。我们的结果强调了 IL-7 作为一种有效的黏膜佐剂的潜力,可刺激 FGT 免疫系统并引发局部免疫接种产生阴道抗体反应,这是预防许多性传播疾病的最有前途的方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ed4a/7947860/7c8e78fc85f4/fimmu-12-614115-g001.jpg

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