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Variation and molecular evolution of HmbR, the Neisseria meningitidis haemoglobin receptor

机译:HMBR的变异与分子演化,Neisseria Meningitidis血红蛋白受体

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Meningococcal disease caused by serogroup B Neisseria meningitidis remains an important health problem in many parts of the world, and there are currently no comprehensive vaccines. Poor immunogenicity, combined with immunological identity to human sialic acids, have hindered the development of a serogroup B conjugate vaccine, resulting in the development of alternative vaccine candidates, including many outer-membrane protein (OMP)-based formulations. However, the design of protein-based meningococcal vaccines is complicated by the high level of genetic and antigenic diversity of the meningococcus. Knowledge of the extent and structuring of this diversity can have implications for the use of particular proteins as potential vaccine candidates. With this in mind, the diversity of the meningococcal OMP HmbR was investigated among N. meningitidis isolates representative of major hyper-invasive lineages. In common with other meningococcal antigens, the genetic diversity of hmbR resulted from a combination of intraspecies horizontal genetic exchange and de novo mutation. Furthermore, genealogical analysis showed an association of hmbR genes with clonal complexes and the occurrence of two hmbR families, A and B. Three variable regions (VR1–VR3), located in loops 2, 3 and 4, were observed with clonal complex structuring of VR types. A minority of codons (3.9?%), located within putative surface-exposed loop regions of a 2D model, were under diversifying selection, indicating regions of the protein likely to be subject to immune attack.
机译:Menisseria Meningitidis血细胞间疾病造成的脑膜炎球菌疾病仍然是世界许多地区的重要健康问题,目前没有全面的疫苗。与人类唾液酸的免疫原性相结合差,已经阻碍了血清群B缀合物疫苗的发育,导致替代疫苗候选物的发展,包括许多外膜蛋白(OMP)的配方。然而,基于蛋白质的脑膜炎球菌疫苗的设计是脑膜炎球菌的高水平遗传和抗原多样性的复杂性。知识这种多样性的程度和结构可以对使用特定蛋白质作为潜在疫苗候选者来说有影响。考虑到这一点,在Nmingitidis分离出代表主要超侵入性谱系的植物中,研究了脑膜炎球菌OMPHMBR的多样性。与其他脑膜炎球菌抗原共同而见,HMBR的遗传多样性是由卧式水平遗传交易所和DE Novo突变的组合产生的。此外,基因分析显示HMBR基因与克隆复合物的缔合,其中克隆复杂结构观察到位于环2,3和4中的三种可变区(VR1-VR3)的三种可变区(VR1-VR3) VR类型。位于2D模型的推定的表面暴露环区域内的少数密码子(3.9?%)在不同的选择下,指示可能受到免疫发作的可能受到免疫发作的区域。

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