AI Article Synopsis
- Hepatitis B virus (HBV) infection is a significant global health issue that can lead to both acute and chronic liver disease, necessitating effective vaccines.
- Researchers are exploring the use of hepatitis B surface-large (HBs-L) antigen in combination with hepatitis B core antigen (HBc) and carboxyl vinyl polymer (CVP) to improve vaccination efficacy against HBV.
- Studies in tree shrews showed that intranasal administration of HBs-L and HBc with CVP significantly enhanced immune responses, indicating potential for both therapeutic and preventive vaccine applications.
Article Abstract
Hepatitis B virus (HBV) infection causes acute and chronic hepatitis, which is a major public health concern worldwide. Immunization methods incorporating hepatitis B surface-small (HBs-S) antigen and hepatitis B core antigen (HBc) have been proposed as candidate therapeutic vaccines, but the elimination of existing HBV infection remains a challenge. To enhance the efficacy of HBs and HBc vaccination, we investigated HBs-large (HBs-L) as an immunogen, and carboxyl vinyl polymer (CVP) as an excipient. HBs-S or HBs-L, in combination with HBc antigen, was administered subcutaneously (without CVP) or intranasally (with or without CVP) for the evaluation of immune response in the tree shrew, which is considered to be a suitable small animal model of HBV infection. Immunization with HBs-L antigen by either route induced a rapid IgG response. Intranasal immunization with HBs-S or HBs-L and HBc formulated with CVP strongly induced neutralizing antibody activity, IgA response, and HBc-specific expression of the interferon gamma-encoding gene. These data indicated the potential of HBs-L and HBc intranasal immunization with CVP, not only as a therapeutic vaccine, but also as a prophylactic vaccine candidate.
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| http://dx.doi.org/10.1016/j.bbrc.2019.09.072 | DOI Listing |
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