Regulation of thymocyte differentiation: pre-TCR signals and β-selection

Abstract

The specificity of the adaptive immune response is, in part, dependent on the clonal expression of the mature T cell receptor (TCR) on T lymphocytes. One mechanism regulating the clonality of the TCR occurs at the level of TCR- β gene rearrangements during lymphocyte development. Expression of a nascent TCR- β chain together with pre-T α (pT α) and CD3 molecules to form the pre-TCR complex, represents a critical checkpoint in T cell differentiation known as β-selection. Indeed, failure to generate a functionally rearranged TCR- β chain at this stage of development results in apoptosis. Signals derived from the pre-TCR complex trigger a maturation program within developing thymocytes that includes: rescue from apoptosis; inhibition of further DNA recombination at the TCR- β gene locus (allowing for the clonality of antigen receptor expression; allelic exclusion); and induction of proliferation and differentiation. The signaling mechanisms that control this developmental program remain largely undefined. Here, we discuss recent evidence investigating the molecular mechanisms that regulate thymocyte differentiation downstream of pre-TCR formation.