Fluctuations in serogroup B meningococcal vaccine antigens prior to routine MenB vaccination in France.

IF 5.4 Q1 MEDICINE, RESEARCH & EXPERIMENTAL Communications medicine Pub Date : 2025-03-25 DOI:10.1038/s43856-025-00800-2
Michaël Falguières, Eva Hong, Mélanie Denizon, Aude Terrade, Muhamed-Kheir Taha, Ala-Eddine Deghmane
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Abstract

Background: Invasive meningococcal disease (IMD) of serogroup B is preventable by protein-based vaccines targeting one (Bivalent rLP2086 vaccine) or several variable proteins (4CMenB vaccine) at the bacterial surface. The 4CMenB was licensed in Europe in 2013 but has been recommended and reimbursed in France for infants over 2 months old since April 2022. The bivalent rLP2086 vaccine was licensed in Europe in 2017 for subjects of 10 years and older. Evaluating strain coverage and fluctuations prior to large scale vaccine use is highly informative.

Methods: We analysed invasive isolates at the French National Reference Centre for meningococci between 1975 and 2022. The 1691 recovered isolates were sequenced. We scored sex, and age groups of subjects. We also scored clonal complexes (CC) and the predicted coverage rates of the corresponding isolates using the genetic Meningococcal Antigen Typing System (gMATS) and the Meningococcal Deduced Vaccine Antigen Reactivity (MenDeVAR).

Results: The period was divided into four periods 1975-1986, 1987-1998-1999-2010 and 2011-2022. Our data clearly show significant differences in the distribution of alleles encoding the vaccine-covered antigens between these four periods. The clonal complex (CC) distribution also differed between the two periods with the disappearance of CC8 since 2011 and drastic decreases in CC11 since 1999. MenDeVar-predicted coverage fluctuated between 46.8% and 60.6% during the four periods for the 4CMenB and between 63.4% and 81.3% for rLP2086. For 4CMenB, coverage was higher using gMATS and varied between 74.5% and 85.0%. Fluctuations were also observed for all age groups.

Conclusions: IMD epidemiology is continuously changing with fluctuation in vaccine strain coverage over the 48 years prior to the routine implementation of the vaccines.

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法国常规B型脑膜炎球菌疫苗接种前血清B型脑膜炎球菌疫苗抗原的波动。
背景:侵袭性脑膜炎球菌病(IMD)可通过蛋白疫苗在细菌表面靶向一种(双价rLP2086疫苗)或几种可变蛋白(4CMenB疫苗)来预防。4CMenB于2013年在欧洲获得许可,但自2022年4月以来,一直在法国推荐并报销2个月以上的婴儿。二价rLP2086疫苗于2017年在欧洲获得许可,用于10岁及以上的受试者。在大规模使用疫苗之前评估毒株覆盖率和波动是非常有用的。方法:我们分析了1975年至2022年间法国国家脑膜炎球菌参考中心的侵袭性分离株。对1691株分离株进行测序。我们对研究对象的性别和年龄组进行了评分。我们还使用遗传脑膜炎球菌抗原分型系统(gMATS)和脑膜炎球菌推定疫苗抗原反应性(MenDeVAR)对克隆复合物(CC)和相应分离物的预测覆盖率进行了评分。结果:研究阶段分为1975 ~ 1986年、1987 ~ 1998 ~ 1999 ~ 2010年和2011 ~ 2022年4个阶段。我们的数据清楚地显示,在这四个时期之间,编码疫苗覆盖抗原的等位基因分布存在显著差异。克隆复合体(CC)的分布也存在差异,自2011年以来CC8消失,而自1999年以来CC11急剧减少。mendevar预测的4CMenB在四个时期的覆盖率在46.8%至60.6%之间波动,rLP2086在63.4%至81.3%之间波动。对于4CMenB,使用gmat的覆盖率更高,在74.5%至85.0%之间变化。在所有年龄组中也观察到波动。结论:在常规实施疫苗之前的48年里,IMD流行病学随着疫苗株覆盖率的波动而不断变化。
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