作者
Anna-Barbara Stittrich, Claudia Haftmann, Evridiki Sgouroudis, Anja Andrea Kühl, Ahmed Nabil Hegazy, Isabel Panse, Rene Riedel, Michael Flossdorf, Jun Dong, Franziska Fuhrmann, Gitta Anne Heinz, Zhuo Fang, Na Li, Ute Bissels, Farahnaz Hatam, Angelina Jahn, Ben Hammoud, Mareen Matz, Felix-Michael Schulze, Ria Baumgrass, Andreas Bosio, Hans-Joachim Mollenkopf, Joachim Grün, Andreas Thiel, Wei Chen, Thomas Höfer, Christoph Loddenkemper, Max Löhning, Hyun-Dong Chang, Nikolaus Rajewsky, Andreas Radbruch, Mir-Farzin Mashreghi
发表日期
2010/11
期刊
Nature immunology
卷号
11
期号
11
页码范围
1057-1062
出版商
Nature Publishing Group US
简介
After being activated by antigen, helper T lymphocytes switch from a resting state to clonal expansion. This switch requires inactivation of the transcription factor Foxo1, a suppressor of proliferation expressed in resting helper T lymphocytes. In the early antigen-dependent phase of expansion, Foxo1 is inactivated by antigen receptor–mediated post-translational modifications. Here we show that in the late phase of expansion, Foxo1 was no longer post-translationally regulated but was inhibited post-transcriptionally by the interleukin 2 (IL-2)-induced microRNA miR-182. Specific inhibition of miR-182 in helper T lymphocytes limited their population expansion in vitro and in vivo. Our results demonstrate a central role for miR-182 in the physiological regulation of IL-2-driven helper T cell–mediated immune responses and open new therapeutic possibilities.
引用总数
学术搜索中的文章
AB Stittrich, C Haftmann, E Sgouroudis, AA Kühl… - Nature immunology, 2010