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

Author:

Lucidarme Jay123,Comanducci Maurizio123,Findlow Jamie123,Gray Stephen J.123,Kaczmarski Edward B.123,Guiver Malcolm123,Vallely Pamela J.123,Oster Philipp123,Pizza Mariagrazia123,Bambini Stefania123,Muzzi Alessandro123,Borrow Ray123

Affiliation:

1. Health Protection Agency, Manchester, United Kingdom

2. Novartis Vaccines, Siena, Italy

3. University of Manchester, Manchester, United Kingdom

Abstract

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%.

Publisher

American Society for Microbiology

Subject

Microbiology (medical),Clinical Biochemistry,Immunology,Immunology and Allergy

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