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DOI: 10.1084/jem.20070618
¤ OpenAccess: Bronze
This work has “Bronze” OA status. This means it is free to read on the publisher landing page, but without any identifiable license.

Bim/Bcl-2 balance is critical for maintaining naive and memory T cell homeostasis

Sara Wojciechowski,Pulak Tripathi,Tristan Bourdeau,Luis Acero,H. Leighton Grimes,Jonathan D. Katz,Fred D. Finkelman,David A. Hildeman

Lymphocytic choriomeningitis
Biology
Homeostasis
2007
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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    Bim/Bcl-2 balance is critical for maintaining naive and memory T cell homeostasis” is a paper by Sara Wojciechowski Pulak Tripathi Tristan Bourdeau Luis Acero H. Leighton Grimes Jonathan D. Katz Fred D. Finkelman David A. Hildeman published in 2007. It has an Open Access status of “bronze”. You can read and download a PDF Full Text of this paper here.