T cells compete for access to antigen-bearing antigen-presenting cells
The Journal of experimental medicine, 2000•rupress.org
These studies tested whether antigenic competition between T cells occurs. We generated
CD8+ T cell responses in H-2b mice against the dominant ovalbumin epitope SIINFEKL
(ova8) and subdominant epitope KRVVFDKL, using either vaccinia virus expressing
ovalbumin (VV-ova) or peptide-pulsed dendritic cells. CD8+ T cell responses were
visualized by major histocompatibility complex class I–peptide tetrameric molecules.
Transfer of transgenic T cells with high affinity for ova8 (OT1 T cells) completely inhibited the …
CD8+ T cell responses in H-2b mice against the dominant ovalbumin epitope SIINFEKL
(ova8) and subdominant epitope KRVVFDKL, using either vaccinia virus expressing
ovalbumin (VV-ova) or peptide-pulsed dendritic cells. CD8+ T cell responses were
visualized by major histocompatibility complex class I–peptide tetrameric molecules.
Transfer of transgenic T cells with high affinity for ova8 (OT1 T cells) completely inhibited the …
These studies tested whether antigenic competition between T cells occurs. We generated CD8+ T cell responses in H-2b mice against the dominant ovalbumin epitope SIINFEKL (ova8) and subdominant epitope KRVVFDKL, using either vaccinia virus expressing ovalbumin (VV-ova) or peptide-pulsed dendritic cells. CD8+ T cell responses were visualized by major histocompatibility complex class I–peptide tetrameric molecules. Transfer of transgenic T cells with high affinity for ova8 (OT1 T cells) completely inhibited the response of host antigen-specific T cells to either antigen, demonstrating that T cells can directly compete with each other for response to antigen. OT1 cells also inhibited CD8+ T cell responses to an unrelated peptide, SIYRYGGL, providing it was presented on the same dendritic cells as ova8. These inhibitions were not due to a more rapid clearance of virus or antigen-presenting cells (APCs) by the OT1 cells. Rather, the inhibition was caused by competition for antigen and antigen-bearing cells, since it could be overcome by the injection of large numbers of antigen-pulsed dendritic cells. These results imply that common properties of T cell responses, such as epitope dominance and secondary response affinity maturation, are the result of competitive interactions between antigen-bearing APC and T cell subsets.
rupress.org
以上显示的是最相近的搜索结果。 查看全部搜索结果