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2008年1月在英格兰和威尔士收集的B群脑膜炎球菌病例分离株中fHbp、nhba(gna2132)、nadA、porA的特征及序列类型,以及一种研究性B群脑膜炎球菌疫苗的潜在覆盖率

Characterization of fHbp, nhba (gna2132), nadA, porA, and sequence type in group B meningococcal case isolates collected in England and Wales during January 2008 and potential coverage of an investigational group B meningococcal vaccine.

作者信息

Lucidarme Jay, Comanducci Maurizio, Findlow Jamie, Gray Stephen J, Kaczmarski Edward B, Guiver Malcolm, Vallely Pamela J, Oster Philipp, Pizza Mariagrazia, Bambini Stefania, Muzzi Alessandro, Borrow Ray

机构信息

Vaccine Evaluation Unit, Health Protection Agency, P.O. Box 209, Floor 2, Clinical Sciences Building 2, Manchester Royal Infirmary, Oxford Road, Manchester M139WZ, United Kingdom.

出版信息

Clin Vaccine Immunol. 2010 Jun;17(6):919-29. doi: 10.1128/CVI.00027-10. Epub 2010 Apr 7.

Abstract

Invasive disease caused by meningococcal capsular groups A, C, W-135, and Y is now preventable by means of glycoconjugate vaccines that target their respective polysaccharide capsules. The capsule of group B meningococci (MenB) is poorly immunogenic and may induce autoimmunity. Vaccines based on the major immunodominant surface porin, PorA, are effective against clonal epidemics but, thus far, have a limited scope of coverage against the wider MenB population at large. In an alternative approach, the first-generation, investigational, recombinant MenB (rMenB) plus outer membrane vesicle (OMV) (rMenB-OMV) vaccine contains a number of relatively conserved surface proteins, fHBP, NHBA (previously GNA2132), and NadA, alongside PorA P1.4-containing OMVs from the New Zealand MeNZB vaccine. MenB currently accounts for approximately 90% of cases of meningococcal disease in England and Wales. To assess potential rMenB-OMV vaccine coverage of pathogenic MenB isolates within this region, all English and Welsh MenB case isolates from January 2008 (n = 87) were genetically characterized with respect to fHBP, NHBA, NadA, and PorA. Alleles for fHbp, nhba, and porA were identified in all of the isolates, of which 22% were also found to harbor nadA alleles. On the basis of genotypic data and predicted immunological cross-reactivity, the potential level of rMenB-OMV vaccine coverage in England and Wales ranges from 66% to 100%.

摘要

由A、C、W-135和Y群脑膜炎球菌引起的侵袭性疾病现在可以通过针对其各自多糖荚膜的糖共轭疫苗来预防。B群脑膜炎球菌(MenB)的荚膜免疫原性较差,可能会诱发自身免疫。基于主要免疫显性表面孔蛋白PorA的疫苗对克隆性流行有效,但迄今为止,对更广泛的MenB总体人群的覆盖范围有限。在另一种方法中,第一代研究性重组MenB(rMenB)加外膜囊泡(OMV)(rMenB-OMV)疫苗包含一些相对保守的表面蛋白,fHBP、NHBA(以前称为GNA2132)和NadA,以及来自新西兰MeNZB疫苗的含PorA P1.4的OMV。目前,MenB在英格兰和威尔士的脑膜炎球菌病病例中约占90%。为了评估该地区致病性MenB分离株的潜在rMenB-OMV疫苗覆盖率,对2008年1月以来所有英格兰和威尔士的MenB病例分离株(n = 87)进行了fHBP、NHBA、NadA和PorA的基因特征分析。在所有分离株中均鉴定出fHbp、nhba和porA的等位基因,其中22%还携带nadA等位基因。根据基因型数据和预测的免疫交叉反应性,rMenB-OMV疫苗在英格兰和威尔士的潜在覆盖率为66%至100%。

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