Productive immune responses require an appropriate environment to support peripheral CD8 + T cell survival. Although host MHC class I molecules appear to be required for this process, the cellular and molecular requirements have not been comprehensively studied. Using adoptive transfer of 2C/recombinase-activating gene-2 (RAG-2) -/-TCR-transgenic T cells, we found that the survival of both naive and effector CD8 + T cells was dependent upon host expression of the same MHC class I alleles that supported thymic selection. Expression of appropriate MHC class I by either bone marrow-or non-bone-marrow-derived cells was sufficient, suggesting that professional antigen-presenting cells were not mandatory. In contrast to MHC class I, neither T cell expression of CD28 nor host expression of ICAM-1 was required for peripheral T cell survival. Finally, T cell death in the absence of appropriate host MHC class I was overcome by elimination of Fas signaling but not by overexpression of Bcl-x L by CD8 + T cells. These results suggest that, in the absence of a survival signal provided by engagement of host MHC/self peptide complexes, CD8 + T cells die via a Fas-dependent, mitochondria-independent pathway.