The PreS-Based Recombinant Vaccine VVX001 Induces Hepatitis B Virus Neutralizing Antibodies in a Low-Responder to HBsAg-Based HBV Vaccines

The PreS-Based Recombinant Vaccine VVX001 Induces Hepatitis B Virus Neutralizing Antibodies in a Low-Responder to HBsAg-Based HBV Vaccines

Approximately 10-20% of subjects vaccinated with HBsAg-based hepatitis B virus (HBV) vaccines are non-responders. BM32 is a recombinant grass pollen allergy vaccine containing the HBV-derived preS surface antigen as an immunological carrier protein. PreS includes the binding site of HBV to its recep...

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Veröffentlicht in:Vaccines (Basel) 2024-09, Vol.12 (10), p.1123
Hauptverfasser: Tulaeva, Inna, Lehmann, Felix, Goldmann, Nora, Dubovets, Alexandra, Trifonova, Daria, Tulaev, Mikhail, Cornelius, Carolin, Weber, Milena, Focke-Tejkl, Margarete, Karaulov, Alexander, Henning, Rainer, Springer, David Niklas, Wiedermann, Ursula, Glebe, Dieter, Valenta, Rudolf
Format: Artikel
Sprache:eng
Schlagworte:
Adjuvants
Allergens
Allergies
Antibodies
Antibody response
Antigens
Binding sites
Carboxyfluorescein diacetate
CD3 antigen
CD4 antigen
Chronic illnesses
Clinical trials
Enzyme-linked immunosorbent assay
Flow cytometry
Genotypes
HBsAg
HBV vaccines
Heparan sulfate
Hepatitis
Hepatitis B
Hepatitis B surface antigen
Hepatocytes
Immunization
Immunoglobulin G
Immunology
Injection
Liver cancer
Lymphocytes
Lymphocytes T
Neutralization
non-responsiveness
Peptides
Pollen
Polypeptides
preS surface protein
Proteins
Vaccines
Yeast
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Zusammenfassung:Approximately 10-20% of subjects vaccinated with HBsAg-based hepatitis B virus (HBV) vaccines are non-responders. BM32 is a recombinant grass pollen allergy vaccine containing the HBV-derived preS surface antigen as an immunological carrier protein. PreS includes the binding site of HBV to its receptor on hepatocytes. We investigated whether immunological non-responsiveness to HBV after repeated HBsAg-based vaccinations could be overcome by immunization with VVX001 (i.e., alum-adsorbed BM325, a component of BM32). A subject failing to develop protective HBV-specific immunity after HBsAg-based vaccination received five monthly injections of 20 µg VVX001. PreS-specific antibody responses were measured by enzyme-linked immunosorbent assay (ELISA) and micro-array technology. Serum reactivity to subviral particles of different HBV genotypes was determined by sandwich ELISA. PreS-specific T cell responses were monitored by carboxyfluorescein diacetate succinimidyl ester (CFSE) staining and subsequent flow cytometry. HBV neutralization was assessed using cultured HBV-infected HepG2 cells. Vaccination with VVX001 induced a strong and sustained preS-specific antibody response composed mainly of the IgG subclass. PreS-specific IgG antibodies were primarily directed to the N-terminal part of preS containing the sodium taurocholate co-transporting polypeptide (NTCP) attachment site. IgG reactivity to subviral particles as well as to the N-terminal preS-derived peptides was comparable for HBV genotypes A-H. A pronounced reactivity of CD3 CD4 lymphocytes specific for preS after the complete injection course remaining up to one year after the last injection was found. Maximal HBV neutralization (98.4%) in vitro was achieved 1 month after the last injection, which correlated with the maximal IgG reactivity to the N-terminal part of preS. Our data suggest that VVX001 may be used as a preventive vaccination against HBV even in non-responders to HBsAg-based HBV vaccines.
ISSN:2076-393X
2076-393X
DOI:10.3390/vaccines12101123