Publication | Open Access
A mouse model of human adaptive immune functions: <i>HLA‐A2.1‐/HLA‐DR1</i>‐transgenic <i>H‐2 class I‐/class II</i>‐knockout mice
137
Citations
39
References
2004
Year
HistocompatibilityTransgenic Mouse ModelsAdaptive Immune SystemHla ImmunogeneticsImmunologyImmune RegulationCd4 T Cell ResponsesHla-dr1-restricted HelperImmune SystemImmunotherapyInflammationImmunogeneticsMouse ModelImmunological MemoryMouse Mhc ResponseAutoimmunityT Cell ImmunityImmune FunctionCell BiologyVaccinationVirus LoadHepatitisHla TypingVaccine DesignMedicine
HLA-A2.1-/HLA-DR1-transgenic H-2 class I-/class II-knockout mice were created and their immunological potential evaluated in response to hepatitis B DNA vaccine. Every single immunized mouse developed hepatitis B virus-specific antibodies, HLA-DR1-restricted helper, and HLA-A2.1-restricted cytolytic T cell responses directed at the same immunodominant epitopes as those identified in naturally infected or vaccinated humans. These mice were specifically protected against a hepatitis B-recombinant vaccinia virus infection with a 10,000-fold or more reduction of the virus load at day 4 post-challenge. These mice represent a unique in vivo experimental model for human immune function studies without any interference with mouse MHC response which dwarfed the prediction of human responses. Furthermore, they enable the complete monitoring of immune adaptative responses for preclinical screening of candidate vaccines.
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