Defective thymocyte proliferation and IL-2 production in transgenic mice expressing a dominant-negative form of CREB

被引：221

作者：

Barton, K

Muthusamy, N

Chanyangam, M

Fischer, C

Clendenin, C

Leiden, JM

机构：

[1] UNIV CHICAGO, DEPT MED, CHICAGO, IL 60637 USA

[2] UNIV CHICAGO, DEPT PATHOL, CHICAGO, IL 60637 USA

来源：

NATURE | 1996年 / 379卷 / 6560期

关键词：

D O I：

10.1038/379081a0

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

THE basic/leucine zipper (bZip) transcription factor, CREB, binds to the CRE element (TGANNTCA)(1-5). The transcriptional activity of CREB requires phosphorylation of the protein on a serine residue at position 119 (ref. 6). CREs are present in a number of T-cell genes(7,8) but the precise role of CREB in T-cell differentiation and function was unknown. Here we show that resting thymocytes contain predominantly unphosphorylated (inactive) CREB, which is rapidly activated by phosphorylation on Ser 119 following thymocyte activation. T-cell development is normal in transgenic mice that express a dominant-negative form of CREB (CREB(A119), with alanine at position 119) under the control of the T-cell-specific CD2 promoter/enhancer. In contrast, thymocytes and T cells from these animals display a profound proliferative defect characterized by markedly decreased interleukin-2 production, G1 cell-cycle arrest and subsequent apoptotic death in response to a number of different activation signals. This proliferative defect is associated with the markedly reduced induction of c-jun, c-fos, Fra-2 and FosB following activation of the CREB(A119), transgenic thymocytes. We propose that T-cell activation leads to the phosphorylation and activation of CREB, which in turn is required for normal induction of the transcription factor AP1 and subsequent interleukin-2 production and cell-cycle progression.

引用

页码：81 / 85

页数：5

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