Restricted appearance of self‐reactive clones into T cell receptor intermediate cells in neonatally thymectomized mice with autoimmune disease

Abstract

Neonatally thymectomized (NTx) mice fall victim to such autoimmune diseases as gastritis and pancreatitis with aging. Self-reactive T cell clones are known to be consistently generated through TCR intermediate (i.e. TCR^int) cell differentiation in normal mice (i.e. via the extrathymic pathways and an alternative intrathymic pathway). It was investigated whether the generation of such clones in NTx mice follows this rule or whether they are generated by default via mainstream T cell differentiation in the thymus. The majority of T cells generated in NTx mice were TCR^int cells in all organs tested. In contrast to athymic mice, which carry only TCR^int cells with aging, a leaky appearance of high TCR (i.e. TCR^hi) cells emerged in the lymph nodes and other organs of NTx mice. Self-reactive clones estimated by anti-Vβ monoclonal antibodies in conjunction with the Mls system were confined to TCR^int cells in all tested organs, including a target organ, the stomach, in NTx mice. A leaky population of TCR^hi cells did not contain a significant number of self-reactive clones. Moreover, such self-reactive clones among TCR^int cells in NTx mice with autoimmune disease were shown to be nonanergic in the proliferation assay. The present results suggest that the generation of self-reactive clones is totally due to TCR^int cell differentiation, although it is still undetermined whether the expanding TCR^int cell population is generated via the extrathymic pathway or an alternative intrathymic pathway. It is shown here not to be due to a failure of the TCR^hi cell-differentiation pathway in NTx mice.