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Bim的缺失导致成熟的CD4-CD8-CD44-CD25-胸腺细胞异常积累。

Loss of Bim results in abnormal accumulation of mature CD4-CD8-CD44-CD25- thymocytes.

作者信息

Hutcheson Jack, Perlman Harris

机构信息

Department of Molecular Microbiology and Immunology, Saint Louis University, School of Medicine, 1402 South Grand Blvd, Saint Louis, MO 63104, USA.

出版信息

Immunobiology. 2007;212(8):629-36. doi: 10.1016/j.imbio.2007.05.003. Epub 2007 Jun 15.

Abstract

The process of thymopoiesis is tightly regulated by a series of selection events which ensure that only functional T-lymphocytes directed against foreign antigens are exported into the periphery. The adaptive immune response largely depends on the regulation of thymocyte development, and thymocytes which fail selection in the thymus are removed by apoptosis. However, the roles of specific apoptotic proteins in early T-lymphocyte development are poorly understood. Here, we report a novel function for Bim in thymocyte development. There is an accumulation of thymocytes in Bim(-/-) mice that lack expression of CD4, CD8, CD44, and CD25 but express CD3 and TCRbeta. Further, the CD4(-)CD8(-)CD25(-)CD44(-)CD3(+)TCRbeta(+) thymocytes are smaller and do not proliferate. These data suggest that these thymocytes are mature DN thymocytes that may have down-regulated the expression of CD4 and CD8. The DN thymocyte phenotype in Bim(-/-) mice is unaffected by the additional loss of Bak or Bax and is similar to the thymic phenotype in mice lacking both Bak and Bax. These data demonstrate that Bim functions to ensure the proper homeostasis of mature thymocytes during selection and thymic export.

摘要

胸腺生成过程受到一系列选择事件的严格调控,这些事件确保只有针对外来抗原的功能性T淋巴细胞输出到外周。适应性免疫反应在很大程度上依赖于胸腺细胞发育的调控,而在胸腺中未能通过选择的胸腺细胞会通过凋亡被清除。然而,特定凋亡蛋白在早期T淋巴细胞发育中的作用仍知之甚少。在此,我们报道了Bim在胸腺细胞发育中的一种新功能。在缺乏CD4、CD8、CD44和CD25表达但表达CD3和TCRβ的Bim(-/-)小鼠中,胸腺细胞出现累积。此外,CD4(-)CD8(-)CD25(-)CD44(-)CD3(+)TCRβ(+)胸腺细胞体积较小且不增殖。这些数据表明,这些胸腺细胞是成熟的双阴性胸腺细胞,可能下调了CD4和CD8的表达。Bim(-/-)小鼠中的双阴性胸腺细胞表型不受Bak或Bax额外缺失的影响,且与同时缺乏Bak和Bax的小鼠的胸腺表型相似。这些数据表明,Bim在选择和胸腺输出过程中发挥作用,以确保成熟胸腺细胞的适当稳态。

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