IL-2 receptor alpha deficient (IL2R^-/-) mice spontaneously accumulate vast numbers of intestinal lamina propria (LP) T cells and develop bowel inflammation. The accumulation of T cells in IL2R^-/- mice is thought to result in part from defective Fas-induced cell death. To understand the role of cell proliferation and death in regulating LP T cells in IL2R^-/- mice, we have directly examined the proliferation and Fas sensitivity of wild-type, lpr/lpr and IL2R^-/- LP T cells. In wild-type mice, BrdU labeling and Fas susceptibility are greatest in CD44^Hi LP T cells. Fas deficient lpr/lpr mice have normal total numbers of LP T cells, despite an increased proportion of BrdU⁺ T cells. By contrast, IL2R^-/- mice possess increased total numbers of LP T cells, despite normal proportions of BrdU⁺ LP T cells. Finally, wild-type and IL2R^-/- LP T cells are equivalently Fas sensitive. These results demonstrate that LP T cells proliferate and are Fas sensitive cells. IL2R^-/- mice accumulate a large number of these Fas sensitive LP T cells, and clearly differ from Fas deficient lpr/lpr mice in this regard. Thus, our studies reveal that Fas is dispensable for LP T cell homeostasis and suggest that the intestinal inflammation observed in IL2R^-/- mice is independent of defective Fas-induced cell death.