2009 年至 2013 年加拿大大西洋地区侵袭性脑膜炎奈瑟菌的特征:特别关注非多糖疫苗目标(PorA、H因子结合蛋白、奈瑟氏肝素结合抗原和奈瑟氏粘附素A)。

Raymond Sw Tsang, Dennis Ks Law, Rita R Gad, Tim Mailman, Gregory German, Robert Needle
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引用次数: 0

摘要

背景:血清 B 群奈瑟氏脑膜炎球菌 (MenB) 一直是加拿大侵袭性脑膜炎球菌疾病 (IMD) 的主要病因。随着 C 型脑膜炎结合疫苗的成功接种,加拿大大多数侵袭性脑膜炎球菌病现在都是由 MenB 引起的:调查 2009 年至 2013 年加拿大大西洋地区的侵袭性脑膜炎病例分离物。分析数据以确定新许可的 MenB 疫苗的潜在覆盖范围:从 IMD 病例分离株中确定血清群、血清型和血清亚型抗原。使用多焦点序列分型进行克隆分析。对基于蛋白质的疫苗抗原基因进行了测序,并对预测的肽进行了研究:大多数 IMD 分离物为 MenB(占 82.5%,40 例中的 33 例),尤其是序列类型 (ST)-154 B:4:P1.4 在加拿大大西洋地区所有 IMD 病例分离物中占 47.5%(40 例中的 19 例)。该克隆的分离株表达了 PorA 抗原 P1.4,并拥有编码奈瑟氏菌肝素结合抗原肽 2 的 nhba 基因,这些基因与新型四联脑膜炎球菌 B 疫苗四种成分中的两种完全吻合。有 19 个 B 型脑膜炎球菌分离物有两个抗原相匹配,另有 5 个 B 型脑膜炎球菌分离物和 1 个 Y 型脑膜炎球菌分离物有一个抗原相匹配。这为 MenB 提供了 75.8% 的潜在覆盖率(33 例中的 25 例),或为 IMD 提供了 62.5% 的总体潜在覆盖率(40 例中的 25 例):2009年至2013年期间,加拿大大西洋地区的IMD主要由MenB引起,尤其是B:4:P1.4 ST-154克隆,占所有IMD病例分离株的47.5%。在加拿大大西洋地区,新的四联脑膜炎球菌B疫苗似乎对MenB有足够的覆盖率。
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Characterization of invasive Neisseria meningitidis from Atlantic Canada, 2009 to 2013: With special reference to the nonpolysaccharide vaccine targets (PorA, factor H binding protein, Neisseria heparin-binding antigen and Neisseria adhesin A).

Background: Serogroup B Neisseria meningitidis (MenB) has always been a major cause of invasive meningococcal disease (IMD) in Canada. With the successful implementation of a meningitis C conjugate vaccine, the majority of IMD in Canada is now caused by MenB.

Objective: To investigate IMD case isolates in Atlantic Canada from 2009 to 2013. Data were analyzed to determine the potential coverage of the newly licensed MenB vaccine.

Methods: Serogroup, serotype and serosubtype antigens were determined from IMD case isolates. Clonal analysis was performed using multilocus sequence typing. The protein-based vaccine antigen genes were sequenced and the predicted peptides were investigated.

Results: The majority of the IMD isolates were MenB (82.5%, 33 of 40) and, in particular, sequence type (ST)-154 B:4:P1.4 was responsible for 47.5% (19 of 40) of all IMD case isolates in Atlantic Canada. Isolates of this clone expressed the PorA antigen P1.4 and possessed the nhba genes encoding for Neisseria heparin-binding antigen peptide 2, which together matched exactly with two of the four components of the new four-component meningococcal B vaccine. Nineteen MenB isolates had two antigenic matches, another five MenB and one meningitis Y isolate had one antigenic match. This provided 75.8% (25 of 33) potential coverage for MenB, or a 62.5% (25 of 40) overall potential coverage for IMD.

Conclusion: From 2009 to 2013, IMD in Atlantic Canada was mainly caused by MenB and, in particular, the B:4:P1.4 ST-154 clone, which accounted for 47.5% of all IMD case isolates. The new four-component meningococcal B vaccine appeared to offer adequate coverage against MenB in Atlantic Canada.

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