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脑膜炎球菌疫苗4CMenB在小鼠阴道感染期间引发针对[原文此处信息缺失]的强烈细胞免疫反应,但并非始终具有保护作用。

Meningococcal vaccine 4CMenB elicits a robust cellular immune response that targets but is not consistently protective against during murine vaginal infection.

作者信息

Zeppa Joseph J, Fegan Jamie E, Maiello Pauline, Islam Epshita A, Lee Isaac S, Pham Christine, Caruso Laura-Lee, Gray-Owen Scott D

机构信息

Department of Molecular Genetics, Temerty Faculty of Medicine, University of Toronto, Toronto, Ontario, Canada.

Department of Microbiology and Molecular Genetics, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania, USA.

出版信息

mSphere. 2025 May 27;10(5):e0094024. doi: 10.1128/msphere.00940-24. Epub 2025 Apr 16.

Abstract

Retrospective epidemiological studies suggest that the licensed serogroup B meningococcal vaccine 4CMenB (Bexsero) provides some protection against the closely related pathogen in humans. This result has been replicated in murine models of gonococcal colonization, with a gonococci-reactive humoral response and more rapid clearance of vaginal infection. However, immunization with 4CMenB consistently elicits a robust humoral response but does not protect all individuals; hence, the correlates of protection remain undefined. Herein, we exploit the fact that 4CMenB promotes gonococcal clearance in only a subset of immunized mice to perform a broad analysis of the adaptive response in animals that are or are not protected. We observe that 4CMenB vaccination induces high levels of anti-neisserial antibodies in both serum and the vaginal lumen, and a robust cellular response highlighted by an increase in both conventional naïve and memory populations as well as unconventional lymphocyte subsets. Multiplex and flow cytometry results show that 4CMenB vaccination generates a robust, multi-faceted cytokine response that spans numerous T cell subsets (T1, T2, T, and T17) and that non-T non-B lymphocytes play an important role in this response, as indicated by an unbiased principal component analysis. Together, this work provides the first comprehensive analysis of the robust humoral and complex cellular response to 4CMenB so as to reveal the effector mechanisms that may contribute to immunity against vaginal gonococcal infection.IMPORTANCEGonorrhea, a sexually transmitted infection caused by the human-specific pathogen (Ngo), is a growing public health concern due to its rise in prevalence and increasing antibiotic resistance against first-line agents. There is currently no vaccine available for this important bacterium due, in part, to our lack of understanding of immune correlates of protection. Interestingly, a human-approved vaccine (4CMenB; Bexsero) against a related pathogen (; a cause of meningitis) has demonstrated some protection against gonorrhea in epidemiologic studies. Herein, we provide the first detailed analysis of cellular and antibody-mediated immune responses to this vaccine in animals protected against gonococcal colonization. These findings provide new understanding regarding immune correlates of protection against , providing new insight into immune protection and helping guide the development of a much-needed vaccine.

摘要

回顾性流行病学研究表明,已获许可的B群脑膜炎球菌疫苗4CMenB(Bexsero)对人类中密切相关的病原体提供了一定程度的保护。这一结果已在淋球菌定植的小鼠模型中得到重现,表现为产生了针对淋球菌的体液免疫反应以及阴道感染清除加快。然而,用4CMenB免疫始终会引发强烈的体液免疫反应,但并不能保护所有个体;因此,保护的相关因素仍不明确。在此,我们利用4CMenB仅能促进部分免疫小鼠清除淋球菌这一事实,对受保护和未受保护动物的适应性反应进行广泛分析。我们观察到,4CMenB疫苗接种可在血清和阴道腔内诱导高水平的抗奈瑟菌抗体,并引发强烈的细胞免疫反应,其特征是传统的初始和记忆细胞群体以及非常规淋巴细胞亚群均有所增加。多重分析和流式细胞术结果表明,4CMenB疫苗接种可产生强大的、多方面的细胞因子反应,涉及众多T细胞亚群(T1、T2、T和T17),并且非T非B淋巴细胞在该反应中发挥重要作用,无偏主成分分析表明了这一点。总之,这项工作首次全面分析了对4CMenB的强烈体液免疫和复杂细胞免疫反应,以揭示可能有助于抵抗阴道淋球菌感染的免疫效应机制。

重要性

淋病是由人类特异性病原体淋病奈瑟菌(Ngo)引起的性传播感染,由于其患病率上升以及对一线药物的抗生素耐药性增加,日益成为公共卫生关注的问题。目前尚无针对这种重要细菌的疫苗,部分原因是我们对保护的免疫相关因素缺乏了解。有趣的是,一种已获人类批准的针对相关病原体(脑膜炎奈瑟菌,脑膜炎的病因)的疫苗(4CMenB;Bexsero)在流行病学研究中已显示出对淋病有一定保护作用。在此,我们首次详细分析了在抵抗淋球菌定植的动物中该疫苗引发的细胞免疫和抗体介导的免疫反应。这些发现为针对淋病奈瑟菌保护的免疫相关因素提供了新的认识,为免疫保护提供了新见解,并有助于指导急需的疫苗的研发。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1bc6/12108064/a6de18fc5318/msphere.00940-24.f001.jpg

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