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- 文献和实验
- 技术资料
- 保存条件:
4°C, stored under nitrogen
- 英文名:
IKK-2 Inhibitor VIII
- 库存:
货期:1-2天
- 供应商:
MedChemExpress LLC
- CAS号:
406209-26-5
- 规格:
10 mM * 1 mL/1 mg/5 mg/10 mg/25 mg/50 mg
| 规格: | 10 mM * 1 mL | 产品价格: | ¥1505.0 |
|---|---|---|---|
| 规格: | 1 mg | 产品价格: | ¥745.0 |
| 规格: | 5 mg | 产品价格: | ¥1368.0 |
| 规格: | 10 mg | 产品价格: | ¥2204.0 |
| 规格: | 25 mg | 产品价格: | ¥4220.0 |
| 规格: | 50 mg | 产品价格: | ¥5244.0 |
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ACHP Hydrochloride
CAS No. : 406209-26-5
MCE 国际站:ACHP Hydrochloride
产品活性:ACHP Hydrochloride (IKK-2 Inhibitor VIII) 是一种有效,选择性的 IKK-β 抑制剂, IC50 为 8.5 nM。
研究领域:NF-κB
作用靶点:IKK
In Vitro: ACHP Hydrochloride (Compound 4j) exhibits potent IKK-β inhibitory (IC50: 8.5 nM) and cellular activities (IC50=40 nM, in A549 cells). ACHP moderately inhibits IKK-α with an IC50 of 250 nM but exhibits good selectivity towards other kinases, such as IKK3, Syk and MKK4 (IC50>20,000 nM). Moreover, ACHP demonstrates quite potent activity in various cellular assays. ACHP inhibits NF-κB-dependent reporter gene activation in TNFα-activated HEK293 cells and PMA/calcium ionophore-activated Jurkat T cells. ACHP fails to inhibit PMA-induced AP-1 activation in MRC-5 cells and PMA/calcium ionophore induced NF-κB dependent reporter gene transcription in Jurkat cells even at concentrations exceeding 10 μM. ACHP selectively interferes with the NF-κB signaling cascade by inhibition of IKK-β in living cells. ACHP inhibits the growth of these cells in a dose-dependent manner. Tax-active cell lines are more susceptible to ACHP than Tax-inactive cell lines and Jurkat (IC50 values in Tax-active cell lines, Tax-inactive cell lines or Jurkat are 3.1±1.3 μM, 10.7±1.7 μM and 23.6 μM, respectively), suggesting that the growth of Tax-active cells depends on NF-κB more than Tax-inactive cells.
In Vivo: ACHP (Compound 4j) is orally bioavailable in mice and rats and demonstrates significant in vivo activity in anti-inflammatory models (arachidonic acid-induced mouse ear edema model). ACHP has reasonable aqueous solubility (0.12 mg/mL in pH 7.4 isotonic buffer) and excellent Caco-2 permeability (Papp 62.3×10-7 cm/s), and demonstrates orally bioavailability in mice (BA: 16%) and rats (BA: 60%). The favourable bioavailability of ACHP in rats is likely due to its low clearance (0.33 L/h/kg). In an acute inflammation model, ACHP exhibits oral efficacy at 1 mg/kg in a dose-dependent manner.
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