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Scand J Infect Dis. 2011 Sep 21. [Epub ahead of print]
A bi-functional hepatitis B virus core antigen (HBcAg) chimera activates
HBcAg-specific T cells and preS1-specific antibodies.
Malik IR, Chen A, Brass A, Ahlén G, Rahman M, Sällberg M, Qureshi JA,
Frelin L.
Source
Department of Laboratory Medicine, Division of Clinical Microbiology,
Karolinska Institutet, Karolinska University Hospital Huddinge , Stockholm
, Sweden.
Abstract
Abstract
A major problem in chronic hepatitis B virus (HBV) infection is
that treatment with specific antivirals is life-long since they rarely
induce a sustained response. An attractive option is therefore to combine
antiviral therapy with some type of immune stimulator, such as a
therapeutic vaccine. Several lines of evidence suggest that a key target
for the cellular immune response is the HBV core antigen (HBcAg). However,
it may also be of advantage to simultaneously improve the neutralizing
antibody response to the surface (S) region of HBV. We therefore generated
chimeric HBcAg particles expressing preS1 residues 1-42 at the tip of the
spike region. We could show that this chimeric HBcAg-preS1 protein primed
both HBcAg-specific T cells and antibodies to preS1. This strongly suggests
that this may be a viable approach to develop an effective bi-functional
therapeutic vaccine as an add-on for the treatment of chronic HBV
infections. |
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发表于 2011-9-28 12:19