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识别艾拉莫德为具有节省类固醇潜力的巨噬细胞移动抑制因子(MIF)抑制剂。

Identification of Iguratimod as an Inhibitor of Macrophage Migration Inhibitory Factor (MIF) with Steroid-sparing Potential.

作者信息

Bloom Joshua, Metz Christine, Nalawade Saisha, Casabar Julian, Cheng Kai Fan, He Mingzhu, Sherry Barbara, Coleman Thomas, Forsthuber Thomas, Al-Abed Yousef

机构信息

From the Hofstra-Northwell School of Medicine, Hempstead, New York 11549,

the Centers for Molecular Innovation.

出版信息

J Biol Chem. 2016 Dec 16;291(51):26502-26514. doi: 10.1074/jbc.M116.743328. Epub 2016 Oct 28.

Abstract

Macrophage migration inhibitory factor (MIF) is a pleiotropic cytokine that has been implicated in a broad range of inflammatory and oncologic diseases. MIF is unique among cytokines in terms of its release profile and inflammatory role, notably as an endogenous counter-regulator of the anti-inflammatory effects of glucocorticoids. In addition, it exhibits a catalytic tautomerase activity amenable to the design of high affinity small molecule inhibitors. Although several classes of these compounds have been identified, biologic characterization of these molecules remains a topic of active investigation. In this study, we used in vitro LPS-driven assays to characterize representative molecules from several classes of MIF inhibitors. We determined that MIF inhibitors exhibit distinct profiles of anti-inflammatory activity, especially with regard to TNFα. We further investigated a molecule with relatively low anti-inflammatory activity, compound T-614 (also known as the anti-rheumatic drug iguratimod), and found that, in addition to exhibiting selective MIF inhibition in vitro and in vivo, iguratimod also has additive effects with glucocorticoids. Furthermore, we found that iguratimod synergizes with glucocorticoids in attenuating experimental autoimmune encephalitis, a model of multiple sclerosis. Our work identifies iguratimod as a valuable new candidate for drug repurposing to MIF-relevant diseases, including multiple sclerosis.

摘要

巨噬细胞移动抑制因子(MIF)是一种多效细胞因子,与多种炎症和肿瘤疾病有关。MIF在细胞因子中在其释放模式和炎症作用方面具有独特性,尤其是作为糖皮质激素抗炎作用的内源性反向调节因子。此外,它具有一种催化互变异构酶活性,适合设计高亲和力小分子抑制剂。尽管已经鉴定出几类这些化合物,但这些分子的生物学特性仍然是一个活跃的研究课题。在本研究中,我们使用体外脂多糖驱动的试验来表征几类MIF抑制剂的代表性分子。我们确定MIF抑制剂表现出不同的抗炎活性谱,特别是在肿瘤坏死因子α方面。我们进一步研究了一种抗炎活性相对较低的分子,化合物T-614(也称为抗风湿药物艾拉莫德),发现除了在体外和体内表现出选择性MIF抑制作用外,艾拉莫德还与糖皮质激素具有相加作用。此外,我们发现艾拉莫德在减轻实验性自身免疫性脑脊髓炎(一种多发性硬化症模型)方面与糖皮质激素协同作用。我们的工作将艾拉莫德确定为一种有价值的新候选药物,可用于重新利用治疗与MIF相关的疾病,包括多发性硬化症。

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