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本帖最后由 StephenW 于 2012-4-5 19:56 编辑
Abstract
| Title | TOWARDS THE DEVELOPMENT OF A THERAPEUTIC VACCINE TO TREAT CHRONIC HBV INFECTION: AD5-BASED VACCINES ENCODING MULTIPLE HBV ANTIGENS INDUCE STRONG T-CELL RESPONSES IN PRE-CLINICAL MODELS | | Speaker: | Geneviève G. Inchauspé | | Author: | P. Martin1, A. Evlachev1, D. Olivier1, C. Beny1, C. Dubois1, A. Findeli2, Y. Schlesinger2, C. Ledoux2, R. Brandely2, T. Menguy2, N. Silvestre2, A. Fournillier1, J.-Y. Bonnefoy3, G. Inchauspé1* | | Affiliation: | 1Infectious Diseases Department, R&D, TRANSGENE SA, Lyon, 2Molecular Immunology Department, R&D, 3R&D, TRANSGENE SA, Illkirch Graffenstaden, France. *[email protected] | Background and aims: Current therapies to treat HBV chronically infected patients are based on IFN-alpha and/or nucleos(t)ide analogs. These are efficient at controlling virus replication but not curing the infection. T cell-mediated immune responses are critical in the spontaneous and therapy-mediated control as well as the resolution of HBV infection. The concept of using active immune-based therapies capable of inducing T-cell responses similar to those seen during control of replication is gaining strong interest and could constitute a novel therapeutic arsenal. We designed an original therapeutic vaccine based on a mix of 2 Adenoviruses encoding 3 HBV antigens (Core, Polymerase and HBsAg domains) and performed pre-clinical studies in a variety of mouse models.
Methods: Adenovirus 5 (Ad5)-based vaccines expressing HBV immunogenic sequences derived from a genotype D isolate were constructed, produced and in vitro characterized by sequencing and western blotting through multiple passages. Immunogenicity studies were performed in two lines of mice (C57Bl6 and HLA-A2 transgenic mice) following sub-cutaneous injections and induced T cell responses were monitored by a panel of assays including ELISPOT IFN-gamma, intracellular cytokine staining, pentamer staining and in vivo cytolysis.
Results: Both Ad5-based vaccines were shown to express the cloned HBV antigens and to be genetically stable. Their ability to induce potent and multispecific CD8-T cell responses (producing IFN-gamma and TNF-alpha and displaying in vivo cytolysis) was demonstrated, when injected alone or as a mix. Vaccine educated CD8-T cells targeted various epitopes derived from the three immunogens including the well-known HLA-A2 Core18-27 epitope associated with resolution. Responses could be boosted following a second administration of the Ad vaccines. In addition, vaccination induced potent cross-reactive CD8-T cells recognizing HBV sequences from genotype B or C (highly prevalent in Asia). This highly immunogenic mix of Ad5-HBV is under evaluation in a HBV transgenic mouse model.
Conclusions: We developed a novel therapeutic adenovirus-based vaccine candidate capable of inducing strong T-cell responses recognizing multiple epitopes and displaying potent cross-reactive potential. A new generation of HBV Ad5-based vaccines aiming at gathering all antigens of interest in one vector is under development. |
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发表于 2012-4-5 19:54
