α-GalCer sp2-Iminoglycolipid Analogs as CD1d-dependent iNKT Modulators: Evaluation of Their Immunotherapeutic Potential in Murine Models of Asthma and Autoimmune Hepatitis

IF 6 2区医学 Q1 CHEMISTRY, MEDICINAL European Journal of Medicinal Chemistry Pub Date : 2024-11-15 DOI:10.1016/j.ejmech.2024.117060

Alan Chuan-Ying Lai, Manuel González-Cuesta, Chieh-Hsin Ho, Po-Yu Chi, Ko-Chien Wu, Gabriel Rocha, Juan C. Muñoz-García, Jesús Angulo, José M. García Fernández, Ya-Jen Chang, Carmen Ortiz Mellet

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Abstract

Invariant natural killer T (iNKT) cells are a subset of innate T cells displaying powerful immunomodulatory functions. Despite extensive preclinical research on the use of iNKT agonist and antagonist for various diseases, translating these findings into successful clinical applications has proven challenging, leaving no approved treatments to date. Efforts to optimize therapeutic outcomes by developing alternative glycolipids to α-galactosylceramide (α-GalCer or KRN7000), the prototypical iNKT antigen, have shown improved preclinical results. However, significant obstacles remain, including the relatively laborious synthesis of α-glycosides and their vulnerability to degradation by α-glycosidases. To overcome these limitations, we explored the use of sp²-iminosugars, a class of glycomimetics, to replace the carbohydrate moiety in α-GalCer-like glycolipids. This substitution offers enhanced biostability and precise control over α-selectivity in glycosylation reactions. The resulting sp²-iminoglycolipids (sp²-IGLs) were tested for their immunomodulatory effects, demonstrating the ability to bind the α-GalCer binding site on the CD1d protein in antigen-presenting cells (APCs), and functioning as iNKT antagonists in α-GalCer-stimulated splenocytes. Notably, analogs featuring a 4-alkyl-1,2,3-aminotriazol-1-yl segment in place of the C₂₅ N-acyl tail in α-GalCer additionally exhibited mild agonistic activity in the absence of α-GalCer stimulation. Computational studies support the formation of stable CD1d– sp²-IGL and CD1d – sp²-IGL – T-cell receptor complexes, with significant differences in the dynamics depending on the glycone nature and lipid tail length. These findings provide a molecular rationale for the observed experimental data. Furthermore, in vivo studies using murine models of asthma and autoimmune hepatitis have identified promising sp²-IGL candidates for further development in immunotherapy.

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作为 CD1d 依赖性 iNKT 调节剂的 α-GalCer sp2 氨基糖脂类似物：在哮喘和自身免疫性肝炎小鼠模型中评估其免疫治疗潜力

不变自然杀伤 T 细胞（iNKT）是先天性 T 细胞的一个亚群，具有强大的免疫调节功能。尽管对 iNKT 激动剂和拮抗剂用于治疗各种疾病进行了广泛的临床前研究，但将这些研究成果成功转化为临床应用却具有挑战性，迄今为止还没有获得批准的治疗方法。通过开发α-半乳糖基甘油酰胺（α-GalCer 或 KRN7000）（iNKT 抗原的原型）的替代糖脂来优化治疗效果，临床前研究结果已有所改善。然而，仍存在一些重大障碍，包括α-糖苷的合成相对费力，而且容易被α-糖苷酶降解。为了克服这些限制，我们探索了使用 sp2-亚氨基糖（一类糖模拟物）来替代 α-GalCer 类糖脂中的碳水化合物。这种取代可提高生物稳定性，并在糖基化反应中精确控制 α 选择性。对由此产生的 sp2-亚氨基糖脂（sp2-IGLs）进行了免疫调节作用测试，结果表明它们能与抗原递呈细胞（APCs）CD1d 蛋白上的α-GalCer 结合位点结合，并在α-GalCer 刺激的脾细胞中发挥 iNKT 拮抗剂的作用。值得注意的是，以 4-烷基-1,2,3-氨基三唑-1-基段代替 α-GalCer 中 C25 N-酰基尾部的类似物在没有 α-GalCer 刺激的情况下也表现出轻微的激动活性。计算研究支持形成稳定的 CD1d- sp2-IGL和CD1d - sp2-IGL-T细胞受体复合物，根据糖元性质和脂质尾长度的不同，复合物的动态也有显著差异。这些发现为观察到的实验数据提供了分子原理。此外，利用小鼠哮喘和自身免疫性肝炎模型进行的体内研究发现了有望进一步开发用于免疫疗法的 sp2-IGL 候选物。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

European Journal of Medicinal Chemistry 化学-医药化学

CiteScore

11.70

自引率

9.00%

发文量

863

审稿时长

29 days

期刊介绍： The European Journal of Medicinal Chemistry is a global journal that publishes studies on all aspects of medicinal chemistry. It provides a medium for publication of original papers and also welcomes critical review papers. A typical paper would report on the organic synthesis, characterization and pharmacological evaluation of compounds. Other topics of interest are drug design, QSAR, molecular modeling, drug-receptor interactions, molecular aspects of drug metabolism, prodrug synthesis and drug targeting. The journal expects manuscripts to present the rational for a study, provide insight into the design of compounds or understanding of mechanism, or clarify the targets.