The roles of MHC class II, CD40, and B7 costimulation in CTL induction by plasmid DNA

K Chan, DJ Lee, A Schubert, CM Tang… - The Journal of …, 2001 - journals.aai.org
K Chan, DJ Lee, A Schubert, CM Tang, B Crain, SP Schoenberger, M Corr
The Journal of Immunology, 2001journals.aai.org
DNA-based vaccines generate potent CTL responses. The mechanism of T cell stimulation
has been attributed to plasmid-transfected dendritic cells. These cells have also been shown
to express plasmid-encoded proteins and to become activated by surface marker up-
regulation. However, the increased surface expression of CD40 and B7 on these dendritic
cells is insufficient to overcome the need for MHC class II-restricted CD4+ T cell help in the
priming of a CTL response. In this study, MHC class II−/− mice were unable to generate a …
Abstract
DNA-based vaccines generate potent CTL responses. The mechanism of T cell stimulation has been attributed to plasmid-transfected dendritic cells. These cells have also been shown to express plasmid-encoded proteins and to become activated by surface marker up-regulation. However, the increased surface expression of CD40 and B7 on these dendritic cells is insufficient to overcome the need for MHC class II-restricted CD4+ T cell help in the priming of a CTL response. In this study, MHC class II−/− mice were unable to generate a CTL response following DNA immunization. This deficit in CTL stimulation by MHC class II-deficient mice was only modestly restored with CD40-activating Ab, suggesting that there were other elements provided by MHC class II-restricted T cell help for CTL induction. CTL activity was also augmented by coinjection with a vector encoding the costimulatory ligand B7. 1, but not B7. 2. These data indicate that dendritic cells in plasmid DNA-injected mice require conditioning signals from MHC class II-restricted T cells that are both CD40 dependent and independent and that there are different roles for costimulatory molecules that may be involved in inducing optimal CTL activity.
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