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Synthetic Glycolipid Ligands for Human iNKT Cells as Potential Therapeutic Agents for Immunotherapy

机译:用于人iNKT细胞的合成糖脂配体作为免疫疗法的潜在治疗剂

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Invariant natural killer T (iNKT) cells are an attractive therapeutic target in autoimmune diseases, since they play a major role in immune regulation. iNKT cells recognize glycolipid antigens presented by CD1d molecules that resemble the non-polymorphic MHC class I protein. α-galactosylceramide (α-GalCer) isolated from marine sponge has long been used as a prototype iNKT cell ligand in the laboratory. As α-GalCer is the most efficacious ligand for iNKT cells, its potential to treat autoimmune disease has been evaluated in animal models. Previous studies showed that α- GalCer effectively suppressed disease in some autoimmunity models, but not in others. This inconsistency may be attributed to the ability of α-GalCer to induce the production of both proinflammatory Th1 and anti-inflammatory Th2 cytokines by iNKT cells. To overcome this issue, we and other groups have synthesized new, unnatural glycolipids by modifying the structure of α-GalCer. These efforts have led to an identification of glycolipid compounds that provoke the production of Th2 (but not Th1) cytokines by iNKT cells. Among these novel ligands, an α-GalCer analogue named OCH, which contains a truncated sphingosine chain, induces a Th2 biased response by murine iNKT cells. Here we describe that OCH also polarizes human iNKT cells towards Th2, which opens up a new avenue for the clinical application of glycolipid compounds in treating of autoimmune diseases such as multiple sclerosis. The pursuit of synthetic glycolipid antigens has the great potential to lead to a better understanding of the regulatory effects of human iNKT cells and development of a new therapeutic agent for autoimmune diseases.
机译:不变的自然杀伤T细胞(iNKT)在自身免疫性疾病中是有吸引力的治疗靶标,因为它们在免疫调节中起主要作用。 iNKT细胞识别类似于非多态性I类MHC蛋白的CD1d分子提供的糖脂抗原。从海洋海绵中分离出的α-半乳糖神经酰胺(α-GalCer)长期以来一直在实验室中用作iNKT细胞配体的原型。由于α-GalCer是iNKT细胞最有效的配体,因此已在动物模型中评估了其治疗自身免疫性疾病的潜力。先前的研究表明,α-GalCer在某些自身免疫模型中可以有效抑制疾病,而在其他一些免疫模型中则不能。这种不一致可以归因于α-GalCer诱导iNKT细胞产生促炎性Th1细胞因子和抗炎性Th2细胞因子的能力。为了克服这个问题,我们和其他小组通过修饰α-GalCer的结构合成了新的非天然糖脂。这些努力导致鉴定出糖脂化合物,这些糖脂化合物可激发iNKT细胞产生Th2(而非Th1)细胞因子。在这些新的配体中,名为OCH的α-GalCer类似物包含一条截短的鞘氨醇链,可诱导鼠iNKT细胞产生Th2偏向反应。在这里,我们描述了OCH还可以使人iNKT细胞向Th2极化,这为糖脂化合物在治疗自身免疫性疾病(如多发性硬化症)中的临床应用开辟了新途径。对合成糖脂抗原的追求具有巨大的潜力,可导致人们更好地了解人iNKT细胞的调节作用,并开发出用于自身免疫疾病的新型治疗剂。

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