Selective expansion of T cells expressing V beta 2 in toxic shock syndrome.

Abstract

Infection with Staphylococcus aureus and the production of toxic shock syndrome toxin-1 (TSST-1) have been implicated in the pathogenesis of toxic shock syndrome. Previous in vitro studies have demonstrated that TSST-1 is a powerful but selective stimulator of human T cells, and that the majority of activated cells express the TCR V.beta.2 gene segment. We therefore studied patients with toxic shock syndrome using a modification of the PCR to determine if expansion of V.beta.2+ T cells is a marker of the in vivo disease process. Five of eight patients studied demonstrated markedly elevated levels of circulating V.beta.2+ T cells, whereas none showed significantly elevated levels of T cells expressing other V.beta. gene segments. The results suggest that toxin-mediated T cell activation, which involves a large fraction of the human T cell repertoire, may be critical in the pathogenesis of this disease.