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恶唑烷酮衍生物洛考他汀可诱导细胞因子缓和。

The oxazolidinone derivative locostatin induces cytokine appeasement.

作者信息

Ménoret Antoine, McAleer Jeremy P, Ngoi Soo-Mun, Ray Swagatam, Eddy Nicholas A, Fenteany Gabriel, Lee Seung-Joo, Rossi Robert J, Mukherji Bijay, Allen David L, Chakraborty Nitya G, Vella Anthony T

机构信息

Department of Immunology, University of Connecticut Health Center, Farmington, CT 06032, USA.

出版信息

J Immunol. 2009 Dec 1;183(11):7489-96. doi: 10.4049/jimmunol.0901414. Epub 2009 Nov 16.

Abstract

Damaging inflammation arising from autoimmune pathology and septic responses results in severe cases of disease. In both instances, anti-inflammatory compounds are used to limit the excessive or deregulated cytokine responses. We used a model of robust T cell stimulation to identify new proteins involved in triggering a cytokine storm. A comparative proteomic mining approach revealed the differential mapping of Raf kinase inhibitory protein after T cell recall in vivo. Treatment with locostatin, an Raf kinase inhibitory protein inhibitor, induced T cell anergy by blocking cytokine production after Ag recall. This was associated with a reduction in Erk phosphorylation. Importantly, in vivo treatment with locostatin profoundly inhibited TNF-alpha production upon triggering the Ag-specific T cells. This effect was not limited to a murine model because locostatin efficiently inhibited cytokine secretion by human lymphocytes. Therefore, locostatin should be a useful therapeutic to control inflammation, sepsis, and autoimmune diseases.

摘要

自身免疫病理和脓毒症反应引发的破坏性炎症会导致严重疾病。在这两种情况下,抗炎化合物都被用于限制过度或失调的细胞因子反应。我们使用了一种强大的T细胞刺激模型来鉴定参与引发细胞因子风暴的新蛋白。一种比较蛋白质组学挖掘方法揭示了体内T细胞再次激活后Raf激酶抑制蛋白的差异图谱。用洛考他汀(一种Raf激酶抑制蛋白抑制剂)处理,通过阻断抗原再次激活后的细胞因子产生来诱导T细胞无反应性。这与Erk磷酸化的减少有关。重要的是,在体内用洛考他汀处理能在触发抗原特异性T细胞时显著抑制TNF-α的产生。这种效应并不局限于小鼠模型,因为洛考他汀能有效抑制人淋巴细胞分泌细胞因子。因此,洛考他汀应该是控制炎症、脓毒症和自身免疫性疾病的一种有用治疗药物。

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