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7α, 25-dihydroxycholesterol-mediated activation of EBI2 in immune regulation and diseases

机译:7α,25-二羟基胆固醇介导的免疫调节和疾病中的EBI2激活

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EBI2, aka GPR183, is a G-couple receptor originally identified in 1993 as one of main genes induced in Burkitt’s lymphoma cell line BL41 by Epstein–Barr virus (EBV) infection. After it was reported in 2009 that the receptor played a key role in regulating B cell migration and responses, we initiated an effort in looking for its endogenous ligand. In 2011 we and another group reported the identification of 7α, 25-dihydroxyxcholesterol (7α, 25-OHC), an oxysterol, as the likely physiological ligand of EBI2. A few subsequently published studies further elucidated how 7α, 25-OHC bound to EBI2, and how a gradient of 7α, 25-OHC could be generated in vivo and regulated migration, activation, and functions of B cells, T cells, dendritic cells (DCs), monocytes/macrophages, and astrocytes. The identification of 7α, 25-OHC as a G protein-coupled receptor ligand revealed a previously unknown signaling system of oxysterols, a class of molecules which exert profound biological functions. Dysregulation of the synthesis or functions of these molecules is believed to contribute to inflammation and autoimmune diseases, cardiovascular diseases, neurodegenerative diseases, cancer as well as metabolic diseases such as diabetes, obesity, and dyslipidemia. Therefore EBI2 may represent a promising target for therapeutic interventions for human diseases.
机译:EBI2,AKA GPR183是最初于1993年鉴定为Burkitt在Burkitt的淋巴瘤(EBV)感染中诱导的主要基因之一的G对接受体。在2009年报道的时候,受体在调节B细胞移民和反应方面发挥了关键作用,我们开始寻找其内源性配体的努力。 2011年,我们和另一组报告鉴定鉴定7α,25-二羟基吡咯(7α,25-OHC),氧气可靠,作为EBI2的可能的生理配体。随后公开的研究进一步阐明了7α,25-OHC结合的eBI2,以及7α,25-OHC的梯度如何在体内产生,并调节B细胞,T细胞,树突细胞的迁移,激活和功能( DCS),单核细胞/巨噬细胞和星形胶质细胞。作为G蛋白偶联受体配体的7α,25-OHC的鉴定揭示了苏西醇的先前未知的信号系统,这是一种施加深刻的生物学功能的分子。据信,这些分子的合成或功能的缺乏造成炎症和自身免疫疾病,心血管疾病,神经变性疾病,癌症以及代谢疾病,如糖尿病,肥胖症和血脂血症。因此,EBI2可以代表人类疾病治疗干预的有希望的靶标。

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