Bim/Bcl-2 balance is critical for maintaining naive and memory T cell homeostasis
S Wojciechowski, P Tripathi, T Bourdeau… - The Journal of …, 2007 - rupress.org
The Journal of experimental medicine, 2007•rupress.org
We examined the role of the antiapoptotic molecule Bcl-2 in combating the proapoptotic
molecule Bim in control of naive and memory T cell homeostasis using Bcl-2−/− mice that
were additionally deficient in one or both alleles of Bim. Naive T cells were significantly
decreased in Bim+/− Bcl-2−/− mice, but were largely restored in Bim−/− Bcl-2−/− mice.
Similarly, a synthetic Bcl-2 inhibitor killed wild-type, but not Bim−/−, T cells. Further, T cells
from Bim+/− Bcl-2−/− mice died rapidly ex vivo and were refractory to cytokine-driven …
molecule Bim in control of naive and memory T cell homeostasis using Bcl-2−/− mice that
were additionally deficient in one or both alleles of Bim. Naive T cells were significantly
decreased in Bim+/− Bcl-2−/− mice, but were largely restored in Bim−/− Bcl-2−/− mice.
Similarly, a synthetic Bcl-2 inhibitor killed wild-type, but not Bim−/−, T cells. Further, T cells
from Bim+/− Bcl-2−/− mice died rapidly ex vivo and were refractory to cytokine-driven …
We examined the role of the antiapoptotic molecule Bcl-2 in combating the proapoptotic molecule Bim in control of naive and memory T cell homeostasis using Bcl-2−/− mice that were additionally deficient in one or both alleles of Bim. Naive T cells were significantly decreased in Bim+/−Bcl-2−/− mice, but were largely restored in Bim−/−Bcl-2−/− mice. Similarly, a synthetic Bcl-2 inhibitor killed wild-type, but not Bim−/−, T cells. Further, T cells from Bim+/−Bcl-2−/− mice died rapidly ex vivo and were refractory to cytokine-driven survival in vitro. In vivo, naive CD8+ T cells required Bcl-2 to combat Bim to maintain peripheral survival, whereas naive CD4+ T cells did not. In contrast, Bim+/−Bcl-2−/− mice generated relatively normal numbers of memory T cells after lymphocytic choriomeningitis virus infection. Accumulation of memory T cells in Bim+/−Bcl-2−/− mice was likely caused by their increased proliferative renewal because of the lymphopenic environment of the mice. Collectively, these data demonstrate a critical role for a balance between Bim and Bcl-2 in controlling homeostasis of naive and memory T cells.
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