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基于 FhbB 的嵌合疫苗的开发,可诱导产生抗体,阻断周围病原体密螺旋体牙龈卟啉单胞菌对因子 H 的结合和切割。

Development of an FhbB based chimeric vaccinogen that elicits antibodies that block Factor H binding and cleavage by the periopathogen Treponema denticola.

机构信息

Department Microbiology and Immunology, Virginia Commonwealth University Medical Center, Richmond, VA, USA.

出版信息

Mol Oral Microbiol. 2021 Feb;36(1):50-57. doi: 10.1111/omi.12325. Epub 2020 Dec 9.

DOI:10.1111/omi.12325
PMID:33219611
Abstract

Treponema denticola is a proteolytic anaerobic spirochete and key contributor to periodontal disease of microbial etiology. As periodontal disease develops and progresses, T. denticola thrives in the hostile environment of the subgingival crevice by exploiting the negative regulatory activity of the complement protein, factor H (FH). FH bound to the cell surface receptor, FhbB (FH binding protein B), is competent to serve as a cofactor for the Factor I mediated-cleavage of the opsonin C3b. However, bound FH is ultimately cleaved by the T. denticola protease, dentilisin. As the T. denticola population expands, the rate of FH cleavage may exceed its rate of replenishment leading to local FH depletion and immune dysregulation culminating in tissue and ligament destruction and tooth loss. The goal of this study was to develop a T. denticola FhbB based-vaccine antigen that can block FH binding and cleavage and kill cells via antibody-mediated bactericidal activity. Tetra (FhbB-ch4) and pentavalent fhbB (FhbB-ch5) chimerics were engineered to have attenuated FH binding ability. The chimerics were immunogenic and elicited high-titer bactericidal and agglutinating antibody. Anti-Fhb-ch4 antisera blocked FH binding and cleavage by the T. denticola protease, dentilisin, in a dose dependent manner. Precedent for the use of FH binding proteins comes from the successful development of two FDA approved vaccines for type B Neiserria meningitidis. This study is the first to extend this approach to the development of a preventive or therapeutic vaccine (or monoclonal Ab) for periodontal disease.

摘要

齿密螺旋体是一种蛋白水解性厌氧螺旋体,是微生物病因牙周病的主要贡献者。随着牙周病的发展和进展,齿密螺旋体在龈下沟的恶劣环境中茁壮成长,利用补体蛋白因子 H (FH)的负调控活性。与细胞表面受体 FhbB(FH 结合蛋白 B)结合的 FH 能够作为因子 I 介导的调理素 C3b 切割的辅助因子。然而,结合的 FH 最终被齿密螺旋体蛋白酶 dentilisin 切割。随着齿密螺旋体种群的扩大,FH 切割的速度可能超过其补充速度,导致局部 FH 耗竭和免疫失调,最终导致组织和韧带破坏和牙齿脱落。本研究的目的是开发一种基于齿密螺旋体 FhbB 的疫苗抗原,该抗原可以阻断 FH 的结合和切割,并通过抗体介导的杀菌活性杀死细胞。四聚体(FhbB-ch4)和五聚体 fhbB(FhbB-ch5)嵌合体被设计为具有减弱的 FH 结合能力。嵌合体具有免疫原性,并引起高滴度的杀菌和凝集抗体。抗 Fhb-ch4 抗血清以剂量依赖的方式阻断齿密螺旋体蛋白酶 dentilisin 对 FH 的结合和切割。FH 结合蛋白的使用先例来自两种已获 FDA 批准的 B 型脑膜炎奈瑟菌疫苗的成功开发。本研究首次将这种方法扩展到牙周病预防性或治疗性疫苗(或单克隆抗体)的开发。

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