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淋病奈瑟菌NHBA和MetQ候选疫苗的改进与优化。

Refinement and optimisation of Neisseria gonorrhoeae NHBA and MetQ vaccine candidates.

作者信息

Eskandari Sharareh, Slesarenko Valentin A, Haselhorst Thomas, Semchenko Evgeny A, Seib Kate L

机构信息

Institute for Biomedicine and Glycomics, Griffith University, Gold Coast, QLD, Australia.

Institute for Biomedicine and Glycomics, Griffith University, Gold Coast, QLD, Australia.

出版信息

Vaccine. 2024 Dec 2;42(26):126416. doi: 10.1016/j.vaccine.2024.126416. Epub 2024 Oct 4.

DOI:10.1016/j.vaccine.2024.126416
PMID:39368128
Abstract

Neisseria gonorrhoeae has a significant impact on reproductive health with an estimated 82 million new cases of infection per year worldwide. Due to the ongoing emergence of multidrug-resistant N. gonorrhoeae strains, the high number of asymptomatic cases, and the risk of disease sequelae, the development of a gonococcal vaccine is urgently needed. We have previously described two potential gonococcal vaccine antigens, cNHBA (C-terminal fragment of the Neisseria Heparin Binding Antigen) and MetQ (methionine-binding protein). This study aimed to optimise these antigens for improved immune responses and to facilitate vaccine production, by investigating cNHBA fusions with the full-length MetQ protein or N-terminal and C-terminal MetQ fragments (Met1 and Met2, respectively) adjuvanted with aluminium hydroxide. The cNHBA and MetQ fragments and fusion antigens were all immunogenic in mice, generating a predominantly IgG1 response. Antibodies mediated bacterial killing via both serum bactericidal activity (SBA) and opsonophagocytic activity (OPA), and reduced adherence to cervical and urethral epithelial cells. Among the antigen fusions tested, MetQ-cNHBA and cNHBA-Met2 generated the highest SBA, OPA and adherence blocking titres and are proposed as promising optimised antigens for N. gonorrhoeae vaccine development.

摘要

淋病奈瑟菌对生殖健康有重大影响,据估计全球每年有8200万新感染病例。由于多重耐药淋病奈瑟菌菌株不断出现、无症状病例数量众多以及疾病后遗症风险,迫切需要开发一种淋病疫苗。我们之前描述了两种潜在的淋病疫苗抗原,即cNHBA(奈瑟菌肝素结合抗原的C端片段)和MetQ(甲硫氨酸结合蛋白)。本研究旨在通过研究cNHBA与全长MetQ蛋白或MetQ的N端和C端片段(分别为Met1和Met2)融合,并佐以氢氧化铝,来优化这些抗原,以改善免疫反应并促进疫苗生产。cNHBA和MetQ片段以及融合抗原在小鼠中均具有免疫原性,主要产生IgG1反应。抗体通过血清杀菌活性(SBA)和调理吞噬活性(OPA)介导细菌杀伤,并减少对宫颈和尿道上皮细胞的粘附。在所测试的抗原融合物中,MetQ-cNHBA和cNHBA-Met2产生了最高的SBA、OPA和粘附阻断效价,并被提议作为淋病奈瑟菌疫苗开发中前景良好的优化抗原。

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