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法国多组份脑膜炎 B 型球菌疫苗(4CMenB)的菌株覆盖率演变。

Evolution of strain coverage by the multicomponent meningococcal serogroup B vaccine (4CMenB) in France.

机构信息

Institute Pasteur, Invasive Bacterial Infections Unit, Paris, France.

GSK, Siena, Italy.

出版信息

Hum Vaccin Immunother. 2021 Dec 2;17(12):5614-5622. doi: 10.1080/21645515.2021.2004055.

DOI:10.1080/21645515.2021.2004055
PMID:34856875
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8903912/
Abstract

The 4CMenB, a protein-based vaccine, was licensed in Europe in 2013 against invasive meningococcal disease caused by serogroup B and is currently implemented in several countries although according to different national strategies. Isolate coverage estimation is required as vaccine-targeted antigens may vary among isolates over time. Several phenotypic and genotypic methods have been developed to predict strain coverage by scoring the expression and cross-reactivity of vaccine antigens using the Meningococcal Antigen Typing system (MATS), by the genetic correlation of alleles encoding these antigens and MATS expression data (gMATS) and by the Meningococcal Deduced Vaccine Antigen Reactivity (MenDeVAR). We applied these approaches on meningococcal B isolates in France and compared two epidemiological years, 2013-2014 and 2018-2019. A strong correlation was observed between MATS data that were generated for the year 2013-2014 and the gMATS data extracted from whole genome sequencing. gMATS and MenDeVAR were next used to compare the two years. Using gMATS, the overall coverage was 77.2% (lower limit (LL)-upper limit (UL) 66.7-87.7) and 70.7% (LL-UL 61.5-80.0) for the two years, respectively. The reduction in coverage between the two years is mainly driven by the reduction of alleles exactly matching the vaccine antigens. A high number of unpredictable isolates was observed using the MenDeVAR and was due to lack of MATS information for new or rare alleles in particular for the year 2018-2019. Our data underline the need of continuous surveillance of strain coverage and the importance of generating phenotypic MATS data to update the genetic approaches of prediction.

摘要

4CMenB 是一种基于蛋白质的疫苗,于 2013 年在欧洲获得许可,可预防由 B 群引起的侵袭性脑膜炎球菌病,目前已在几个国家实施,尽管实施策略各不相同。由于疫苗靶向抗原在不同时间的分离株中可能存在差异,因此需要进行分离株覆盖率估计。已经开发了几种表型和基因型方法来预测菌株覆盖率,方法是使用脑膜炎球菌抗原分型系统 (MATS) 对疫苗抗原的表达和交叉反应进行评分,通过编码这些抗原的等位基因的遗传相关性和 MATS 表达数据 (gMATS),以及通过脑膜炎球菌推导疫苗抗原反应性 (MenDeVAR)。我们将这些方法应用于法国的脑膜炎球菌 B 分离株,并比较了两个流行病学年份,2013-2014 年和 2018-2019 年。观察到 2013-2014 年生成的 MATS 数据与从全基因组测序中提取的 gMATS 数据之间存在很强的相关性。接下来,使用 gMATS 和 MenDeVAR 比较这两年的数据。使用 gMATS,两年的总体覆盖率分别为 77.2%(下限(LL)-上限(UL)66.7-87.7)和 70.7%(LL-UL 61.5-80.0)。两年之间覆盖率的降低主要是由于与疫苗抗原完全匹配的等位基因的减少。使用 MenDeVAR 观察到大量不可预测的分离株,这主要是由于缺乏针对新的或罕见等位基因的 MATS 信息,特别是在 2018-2019 年。我们的数据强调了需要对菌株覆盖率进行持续监测,以及生成表型 MATS 数据以更新预测的遗传方法的重要性。

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2
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