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携带分枝杆菌Ag85B-ESAT-6抗原在不同细胞定位时的免疫原性特性比较。

Comparison of the Immunogenic Properties of Carrying the Mycobacterial Ag85B-ESAT-6 Antigen at Various Cellular Localizations.

作者信息

Wiull Kamilla, Boysen Preben, Kuczkowska Katarzyna, Moen Lars Fredrik, Carlsen Harald, Eijsink Vincent G H, Mathiesen Geir

机构信息

Faculty of Chemistry, Biotechnology and Food Science, NMBU - Norwegian University of Life Sciences, Ås, Norway.

Faculty of Veterinary Medicine, NMBU - Norwegian University of Life Sciences, Ås, Norway.

出版信息

Front Microbiol. 2022 Jun 3;13:900922. doi: 10.3389/fmicb.2022.900922. eCollection 2022.

Abstract

The bacille Calmette-Guèrin (BCG) vaccine has been used for a century; nonetheless, tuberculosis (TB) remains one of the deadliest diseases in the world. Thus, new approaches to developing a new, more efficient vaccine are desirable. Mucosal vaccines are of particular interest, considering that first enters the body through the mucosal membranes. We have previously demonstrated the immunogenicity of a recombinant delivery vector with TB hybrid antigen Ag85B-ESAT-6 anchored to the cell membrane. The goal of the present study was to analyze the impact of antigen localization in the immune response. Thus, we assessed two novel vaccine candidates, with the TB antigen either non-covalently anchored to the cell wall (LysMAgE6) or located intracellularly (CytAgE6). In addition, we compared two expression systems, using an inducible (LipoAgE6) or a constitutive promoter (LipoAgE6) for expression of covalently anchored antigen to the cell membrane. Following administration to mice, antigen-specific CD4 T-cell proliferation and IFN-γ and IL-17A secretion were analyzed for lung cell and splenocyte populations. Generally, the immune response in lung cells was stronger compared to splenocytes. The analyses showed that the type of expression system did not significantly affect the immunogenicity, while various antigen localizations resulted in markedly different responses. The immune response was considerably stronger for the surface-displaying candidate strains compared to the candidate with an intracellular antigen. These findings emphasize the significance of antigen exposure and further support the potential of as a mucosal vaccine delivery vehicle in the fight against TB.

摘要

卡介苗(BCG)疫苗已使用了一个世纪;尽管如此,结核病(TB)仍然是世界上最致命的疾病之一。因此,开发一种新的、更有效的疫苗的新方法是可取的。考虑到结核菌首先通过黏膜进入人体,黏膜疫苗尤其令人关注。我们之前已经证明了一种重组递送载体的免疫原性,该载体将结核杂交抗原Ag85B - ESAT - 6锚定在细胞膜上。本研究的目的是分析抗原定位对免疫反应的影响。因此,我们评估了两种新型候选疫苗,一种是结核抗原非共价锚定在细胞壁上(LysMAgE6),另一种是位于细胞内(CytAgE6)。此外,我们比较了两种表达系统,一种使用诱导型启动子(LipoAgE6),另一种使用组成型启动子(LipoAgE6)来表达共价锚定在细胞膜上的抗原。给小鼠接种后,分析了肺细胞和脾细胞群体中抗原特异性CD4 T细胞增殖以及IFN - γ和IL - 17A的分泌情况。一般来说,与脾细胞相比,肺细胞中的免疫反应更强。分析表明,表达系统的类型对免疫原性没有显著影响,而不同的抗原定位导致了明显不同的反应。与具有细胞内抗原的候选疫苗相比,表面展示候选菌株的免疫反应要强得多。这些发现强调了抗原暴露的重要性,并进一步支持了[载体名称]作为抗结核黏膜疫苗递送载体的潜力。 (注:原文中“first enters the body through the mucosal membranes”前的“first”指代不明;“while various antigen localizations resulted in markedly different responses”前缺少“while”,可能会影响句子理解,翻译时按原意尽量通顺表达。“[载体名称]”指代原文中未明确的相关载体)

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f627/9204040/4ac96002eab6/fmicb-13-900922-g001.jpg

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