Mutations affecting the Tec kinases Itk and Rlk decrease T cell receptor-induced Ca
2+ mobilization and Erk kinase activation and impair both positive and negative thymic selection.
Itk
−/−
and
Rlk
...−/−Itk
−/−
mice also have decreased CD4:8 T cell ratios, suggestive of altered CD4:8 lineage commitment. Nonetheless, we find that CD8 single-positive (SP) thymocytes and peripheral CD8
+ T cells in these mice do not resemble conventional CD8
+ T cells. Instead, these cells express memory markers, rapidly produce interferon-γ, and can be selected on hematopoietically derived cells, similar to MHC class Ib-restricted “innate-type” lymphocytes. Itk deficiency also greatly increases the number of cells selected by MHC class Ib. Expression of a hypersensitive Erk2 mutant partially corrects the CD8
+ T cell phenotypes in
Itk
−/−
mice, arguing that altered signaling permits development of this innate-type CD8
+ cell population. Our results suggest that Tec kinases differentially regulate development of conventional versus nonconventional lymphocytes.
Mutations affecting the Tec kinases Itk and Rlk decrease T cell receptor- induced Ca super(2+) mobilization and Erk kinase activation and impair both positive and negative thymic selection. Itk ...super(-/-) and Rlk super(-/-)Itk super(-/-) mice also have decreased CD4:8 T cell ratios, suggestive of altered CD4:8 lineage commitment. Nonetheless, we find that CD8 single-positive (SP) thymocytes and peripheral CD8 super(+) T cells in these mice do not resemble conventional CD8 super(+) T cells. Instead, these cells express memory markers, rapidly produce interferon- gamma , and can be selected on hematopoietically derived cells, similar to MHC class Ib-restricted "innate-type" lymphocytes. Itk deficiency also greatly increases the number of cells selected by MHC class Ib. Expression of a hypersensitive Erk2 mutant partially corrects the CD8 super(+) T cell phenotypes in Itk super(-/-) mice, arguing that altered signaling permits development of this innate-type CD8 super(+) cell population. Our results suggest that Tec kinases differentially regulate development of conventional versus nonconventional lymphocytes.
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