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Differences in the population structure of Neisseria meningitidis in two Australian states: Victoria and Western Australia

机译:澳大利亚两个州的维多利亚州和西澳大利亚州脑膜炎奈瑟氏球菌的人口结构差异

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摘要

Neisseria meningitidis is the causative agent of invasive meningococcal disease (IMD). A recombinant vaccine called Bexsero® incorporates four subcapsular antigens (fHbp, NHBA, NadA and PorA) which are used to assign a Bexsero® antigen sequence type (BAST) to each meningococcal strain. The vaccine elicits an immune response against combinations of variants of these antigens which have been grouped into specific BAST profiles that have been shown to have different distributions within geographical locations thus potentially affecting the efficacy of the vaccine. In this study, invasive meningococcal disease isolates from the western seaboard of Australia (Western Australia; WA) were compared to those from the south-eastern seaboard (Victoria; VIC) from 2008 to 2012. Whole-genome sequencing (WGS) of 131 meningococci from VIC and 70 meningococci from WA were analysed for MLST, FetA and BAST profiling. Serogroup B predominated in both jurisdictions and a total of 10 MLST clonal complexes (cc) were shared by both states. Isolates belonging to cc22, cc103 and cc1157 were unique to VIC whilst isolates from cc60 and cc212 were unique to WA. Clonal complex 41/44 represented one-third of the meningococcal population in each state but the predominant ST was locally different: ST-6058 in VIC and ST-146 in WA. Of the 108 BAST profiles identified in this collection, only 9 BASTs were simultaneously observed in both states. A significantly larger proportion of isolates in VIC harboured alleles for the NHBA-2 peptide and fHbp-1, antigenic variants predicted to be covered by the Bexsero® vaccine. The estimate for vaccine coverage in WA (47.1% [95% CI: 41.1–53.1%]) was significantly lower than that in VIC (66.4% [95% CI: 62.3–70.5%]). In conclusion, the antigenic structure of meningococci causing invasive disease in two geographically distinct states of Australia differed significantly during the study period which may affect vaccine effectiveness and highlights the need for representative surveillance when predicting potential impact of meningococcal B vaccines.
机译:脑膜炎奈瑟氏球菌是侵袭性脑膜炎球菌病(IMD)的病原体。一种称为Bexsero ®的重组疫苗掺入了四个亚荚膜抗原(fHbp,NHBA,NadA和PorA),用于为每个脑膜炎球菌分配Bexsero 抗原序列类型(BAST)应变。疫苗引发针对这些抗原变体组合的免疫应答,这些抗原变体已被分组为特定的BAST图谱,这些图谱显示在地理位置上具有不同的分布,因此可能影响疫苗的功效。在这项研究中,比较了2008年至2012年澳大利亚西部沿海地区(西澳大利亚州;华盛顿州)与东南沿海地区(维多利亚州;维多利亚州)的侵袭性脑膜炎球菌分离株。131例脑膜炎球菌的全基因组测序(WGS)对来自VIC的来自MIC和来自WA的70个脑膜炎球菌进行了MLST,FetA和BAST分析。血清型B在两个辖区均占主导地位,两国共有10个MLST克隆复合体(cc)。属于cc22,cc103和cc1157的分离株是VIC独有的,而来自cc60和cc212的分离株则是WA独有的。每种情况下,克隆复合物41/44代表脑膜炎球菌人口的三分之一,但主要的ST局部不同:VIC中的ST-6058和WA中的ST-146。在该集合中鉴定出的108个BAST配置文件中,在两种状态下仅同时观察到9个BAST。在VIC中,有很大比例的分离株带有NHBA-2肽和fHbp-1等位基因,这些抗原变体预计将被Bexsero ®疫苗覆盖。西澳大利亚州的疫苗覆盖率估计值(47.1%[95%CI:41.1–53.1%])显着低于VIC(66.4%[95%CI:62.3–70.5%])。总之,在研究期间,澳大利亚两个地理上不同的州引起脑膜炎球菌侵袭性疾病的抗原结构存在显着差异,这可能影响疫苗的有效性,并突出了在预测脑膜炎球菌B疫苗的潜在影响时需要进行代表性监测的必要性。

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