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Conservation of Meningococcal Antigens in the Genus Neisseria

机译:奈瑟菌属中脑膜炎球菌抗原的保守性

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Neisseria meningitidis, one of the major causes of bacterial meningitis and sepsis, is a member of the genus Neisseria, which includes species that colonize the mucosae of many animals. Three meningococcal proteins, factor H-binding protein (fHbp), neisserial heparin-binding antigen (NHBA), and N. meningitidis adhesin A (NadA), have been described as antigens protective against N.?meningitidis of serogroup B, and they have been employed as vaccine components in preclinical and clinical studies. In the vaccine formulation, fHbp and NHBA were fused to the GNA2091 and GNA1030 proteins, respectively, to enhance protein stability and immunogenicity. To determine the possible impact of vaccination on commensal neisseriae, we determined the presence, distribution, and conservation of these antigens in the available genome sequences of the genus Neisseria, finding that fHbp, NHBA, and NadA were conserved only in species colonizing humans, while GNA1030 and GNA2091 were conserved in many human and nonhuman neisseriae. Sequence analysis showed that homologous recombination contributed to shape the evolution and distribution of both NHBA and fHbp, three major variants of which have been defined. fHbp variant 3 was probably the ancestral form of meningococcal fHbp, while fHbp variant 1 from N.?cinerea was introduced into N.?meningitidis by a recombination event. fHbp variant 2 was the result of a recombination event inserting a stretch of 483?bp from variant 1 into the variant 3 background. These data indicate that a high rate of exchange of genetic material between neisseriae that colonize the human upper respiratory tract exists. >IMPORTANCE The upper respiratory tract of healthy individuals is a complex ecosystem colonized by many bacterial species. Among these, there are representatives of the genus Neisseria, including Neisseria?meningitidis, a major cause of bacterial meningitis and sepsis. Given the close relationship between commensal and pathogenic species, a protein-based vaccine against N.?meningitidis has the potential to impact the other commensal species of Neisseria. For this reason, we have studied the distribution and evolutionary history of the antigen components of a recombinant vaccine, 4CMenB, that recently received approval in Europe under the commercial name of Bexsero?. We found that fHbp, NHBA, and NadA can be found in some of the human commensal species and that the evolution of these antigens has been essentially shaped by the high rate of genetic exchange that occurs between strains of neisseriae that cocolonize the same environment.
机译:脑膜炎奈瑟氏球菌是细菌性脑膜炎和败血症的主要原因之一,是脑膜炎奈瑟氏菌属的成员,其中包括许多动物的黏膜定居的物种。三个脑膜炎球菌蛋白,因子H结合蛋白(fHbp),奈瑟氏肝素结合抗原(NHBA)和 N 。脑膜炎奈瑟菌粘附素A(NadA)被描述为针对血清群B的脑膜炎奈瑟菌的保护性抗原,在临床前和临床研究中已被用作疫苗成分。在疫苗制剂中,将fHbp和NHBA分别融合到GNA2091和GNA1030蛋白上,以增强蛋白的稳定性和免疫原性。为了确定疫苗接种对共代奈瑟菌的可能影响,我们确定了奈瑟菌属的可用基因组序列中这些抗原的存在,分布和保守性,发现fHbp,NHBA和NadA均被保守。 GNA1030和GNA2091在许多人类和非人类奈瑟菌中都是保守的。序列分析表明同源重组有助于塑造NHBA和fHbp的进化和分布,已确定了它们的三个主要变体。 fHbp变体3可能是脑膜炎球菌fHbp的祖先形式,而 cinerea N.cinerea 的fHbp变体1通过重组事件被引入到 meningitidis 中。 fHbp变异体2是重组事件的结果,该重组事件将来自变异体1的483?bp片段插入变异体3背景。这些数据表明在人类上呼吸道定殖的奈瑟氏球菌之间存在遗传物质的高交换率。 >重要:健康个体的上呼吸道是一个复杂的生态系统,周围遍布着许多细菌。其中,有奈瑟球菌属,包括 Neisseria?meningitidis ,这是细菌性脑膜炎和败血症的主要原因。鉴于共生病原菌与致病菌之间的密切关系,针对蛋白的 N.meningitidis 疫苗可能会影响其他 Neisseria 共生菌。因此,我们研究了重组疫苗4CMenB的抗原成分的分布和进化史,该疫苗最近在欧洲以商品名Bexsero?获得批准。我们发现fHbp,NHBA和NadA可以在某些人类共生物种中发现,而这些抗原的进化基本上是由在同一环境下进行结肠炎的奈瑟氏球菌菌株之间发生的高遗传交换率所决定的。

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