The role of major histocompatibility complex (MHC) molecules in T cell
differentiation was investigated by comparison of thymocyte subpopula
tions in wild-type mice and beta2-microglobulin (beta2M) mutant mice d
eficient in MHC class I expression and mature CD8+ cells. On the basis
of surface markers, glucocorticoid resistance, in vitro differentiati
on capacity, and absence in beta2M-/- mice, CD4(intermediate)CD8hi cel
ls with high expression of alphabeta T cell receptor (TCRalphabeta) we
re identified as having been positively selected by MHC class I for de
velopment into mature CD8+ T cells. Activated CD4(int)CD8hi cells bear
ing intermediate rather than high amounts of TCR were present in both
wild-type and beta2M-/- animals. These data suggest that recognition o
f MHC class I molecules is required for full maturation to CD8+ T cell
s, but not for receptor-initiated commitment to the CD8+ lineage, cons
istent with a stochastic (selection) model of thymocyte development.