S1P(1)受体激动剂:选择性和当前临床活性评估

Kevin P Cusack, Robert H Stoffel
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引用次数: 0

摘要

自从发现芬戈莫德(FTY-720)诱导淋巴细胞减少的作用机制与S1P GPCR家族有关以来,人们对鞘氨醇-1-磷酸(S1P)受体激动剂的兴趣稳步增加。芬戈莫德是5种S1P家族受体中的4种受体的激动剂。过继细胞转移实验和选择性S1P(1)受体激动剂证明,S1P(1)受体是次要淋巴组织中捕获淋巴细胞的主要靶点。这种易于获取、可翻译的生物标志物与免疫疾病啮齿动物模型的疗效相关。诺华公司于2009年12月在美国和欧盟申请批准芬戈莫德用于治疗多发性硬化症。此外,多家公司针对S1P受体的选择性化合物已进入临床试验阶段。这些化合物可分为两类S1P(1)受体激动剂:氨基醇前药和第二代直接激动剂。本文就该类化合物的研究进展及其在S1P受体家族选择性中的作用作一综述。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
S1P(1) receptor agonists: Assessment of selectivity and current clinical activity.

Interest in sphingosine-1-phosphate (S1P)(1) receptor agonists has increased steadily since the discovery that the mechanism of action of fingolimod (FTY-720)-induced lymphopenia is linked to the S1P GPCR family. Fingolimod is an agonist at four out of the five S1P family receptors. Adoptive cell transfer experiments and selective S1P(1) receptor agonists provided evidence that the S1P(1) receptor is the main target responsible for trapping lymphocytes in secondary lymphoid tissue. This readily accessible, translatable biomarker has been correlated with efficacy in rodent models of immune disease. Novartis AG filed for regulatory approval for fingolimod in the US and EU for the treatment of multiple sclerosis in December 2009. In addition, more selective compounds targeting S1P receptors from several companies have entered clinical trials. These compounds can be categorized into two classes of S1P(1) receptor agonists: amino alcohol prodrugs and second-generation direct agonists. This review focuses on the development of these compounds and the role of S1P receptor family selectivity.

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