| Description |
ACT-777991 is an orally active and selective CXCR3 antagonist. ACT-777991 has microsomes and hepatocytes stability across animal models. ACT-777991 inhibits the migration of activated T cells toward CXCL11[1].
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| Related Catalog |
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| Target |
CXCR3
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| In Vitro |
ACT-777991 在 CHO 细胞中抑制 hEGR,IC50 值为 26 μM[1]。 ACT-777991(1 μM;45 分钟)在人类、大鼠和狗的微粒体和肝细胞中稳定[1]。 ACT-777991(0.01-1 μM)抑制人和小鼠激活的 T 细胞向 CXCL11 的迁移,IC50 范围分别为 3.2-64 nM 和 4.9-21 nM[1]。 ACT-777991(1 nM、5 nM、20 nM 和 50 nM)抑制 CXCR3 介导的人和小鼠 T 细胞趋化性[1]。
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| In Vivo |
ACT-777991(0.5 mg/kg,1 mg/kg;静脉注射;单次剂量)在雄性 Wistar 大鼠 (14/156) 或 Beagle 犬 (5/15) 中具有低体内血浆清除率[1]。 ACT-777991(0.006-2 mg/g 食物;口服;在 LPS 处理前 3 天开始给药,LPS 处理后 72 小时结束)剂量依赖性地抑制小鼠模型体内 CXCR3+ T 细胞的趋化性[1]。 Animal Model: LPS challenge model in mice[1] Dosage: 0.006, 0.02, 0.06, 0.2, 0.6, and 2 mg per g of food Administration: PO; started 3 days before LPS challenge and continued up to the end of the study (72 h post LPS challenge) Result: Reduced the number of BAL CD8+ T cells in a dose-dependent manner.
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| References |
[1]. Meyer EA, et al. Discovery of Clinical Candidate ACT-777991, a Potent CXCR3 Antagonist for Antigen-Driven and Inflammatory Pathologies. J Med Chem. 2023 Mar 23;66(6):4179-4196.
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