Common regulation of apoptosis signaling induced by CD95 and the DNA- damaging stimuli etoposide and γ-radiation downstream from caspase-8 activation

Abstract

The death receptor CD95 (APO-1/Fas), the anticancer drug etoposide, and γ-radiation induce apoptosis in the human T cell line Jurkat. Variant clones selected for resistance to CD95-induced apoptosis proved cross-resistant to etoposide- and radiation-induced apoptosis, suggesting that the apoptosis pathways induced by these distinct stimuli have critical component(s) in common. The pathways do not converge at the level of CD95 ligation or caspase-8 signaling. Whereas caspase-8 function was required for CD95- mediated cytochrome c release, effector caspase activation, and apoptosis, these responses were unaffected in etoposide-treated and irradiated cells when caspase-8 was inhibited by FLIP(L). Both effector caspase processing and cytochrome c release were inhibited in the resistant variant cells as well as in Bcl-2 transfectants, suggesting that, in Jurkat cells, the apoptosis signaling pathways activated by CD95, etoposide, and γ-radiation are under common mitochondrial control. All three stimuli induced ceramide production in wild-type cells, but not in resistant variant cells. Exogenous ceramide bypassed apoptosis resistance in the variant cells, but not in Bcl-2- transfected cells, suggesting that apoptosis signaling induced by CD95, etoposide, and γ-radiation is subject to common regulation at a level different from that targeted by Bcl-2.