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S83344

AM-2099

源叶(MedMol) 98%
  • 英文名:
  • AM-2099
  • 别名:
  • CAS号:
  • 1443373-17-8
  • 分子式:
  • C19H13F3N4O3S2
  • 分子量:
  • 466.4567
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源叶(MedMol) S83344-5mg 98% ¥2200.00元 预计交期:2-3天 - - - EA 加入购物车
源叶(MedMol) S83344-10mg 98% ¥3900.00元 预计交期:2-3天 - - - EA 加入购物车
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  • 提示:详情请下载说明书。
  • 产品描述: AM-2099 is a potent and selective inhibitor of voltage-gated sodium channel Nav1.7 with an IC50 of 0.16 μM for human Nav1.7.
  • 靶点: IC50: 0.16 μM (human Nav1.7), 0.18 μM (mouse Nav1.7), 3.5 μM (rat Nav1.7);Others
  • 体外研究:
    In heterologous cells, comparable inhibition is observed across human, mouse, dog, and cynomolgus monkey NaV1.7 with reduced activity against rat NaV1.7. AM-2099 is more than 100-fold selective over Nav1.3, Nav1.4, Nav1.5, and Nav1.8, while lower levels of selectivity are observed against Nav1.1, Nav1.2, and Nav1.6. AM-2099 demonstrates low affinity for hERG (>30 µM) and does not show greater than 50% inhibition against a panel of 100 kinases (1 µM) and a broad CEREP panel (10 µM).
  • 体内研究:
    AM-2099 demonstrates a favorable pharmacokinetic profile in rat and dog. In rats AM-2099 shows low total clearance and moderate Vdss and half-life. In contrast, when dosed in dogs AM-2099 shows very low clearance, a low Vdss and long halflife (18 h). AM-2099 demonstrates a dose-dependent increase in plasma exposure with a concomitant dose-dependent reduction in scratching bouts compared to vehicle-treated animals, with a statistically significant reduction observed at the 60 mg/kg dose
  • 参考文献:
    1. Marx IE, et al. Sulfonamides as Selective NaV1.7 Inhibitors: Optimizing Potency and Pharmacokinetics to Enable in Vivo Target Engagement. ACS Med Chem Lett. 2016 Sep 21;7(12):1062-1067.
  • 溶解性: soluble  in  DMSO
  • 保存条件: -20℃
  • 配置溶液浓度参考:
    1mg 5mg 10mg
    1 mM 2.144 ml 10.719 ml 21.438 ml
    5 mM 0.429 ml 2.144 ml 4.288 ml
    10 mM 0.214 ml 1.072 ml 2.144 ml
    50 mM 0.043 ml 0.214 ml 0.429 ml
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