CD4 assists in T cell recognition of peptides bound to MHC class II molecules by binding to a non-polymorphic region on class II and stabilizing TCR recognition of the peptide-class II complex. Overexpression of CD4 in transgenic mice expressing a class II-restricted TCR resulted in a dramatic loss of thymocytes that became evident soon after the TCR and CD4 were co-expressed. Both the thymus and lymph nodes of the double-transgenic mice had reduced numbers of CD4 lineage T cells. A large proportion of the remaining CD4 lineage T cells lost either the transgenic TCR alpha or beta chains. The double-transgenic mice continued to generate thymocytes and T cells that expressed the transgenic TCR, but these cells did not express endogenous CD4. Overexpression of CD4 thus severely disrupts the normal developmental pathway of these thymocytes, supporting a model in which avidity of the TCR complex for self class II molecules determines the outcome of thymocyte development.