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Drinabant
CAS No. 358970-97-5
Drinabant ( AVE-1625 )
产品货号. M27478 CAS No. 358970-97-5
Drinabant 是一种口服活性 CB1 受体拮抗剂。 Drinabant 抑制激动剂刺激的钙信号,对 hCB1-R 和 rCB1-R 的 IC50 值分别为 25 nM 和 10 nM,对 hCB2-R 无效。
纯度: >98% (HPLC)
COA
Datasheet
HNMR
HPLC
MSDS
Handing Instructions
| 规格 | 价格/人民币 | 库存 | 数量 |
| 2MG | ¥1596 | 有现货 |
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| 5MG | ¥2406 | 有现货 |
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| 10MG | ¥3686 | 有现货 |
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| 25MG | ¥6059 | 有现货 |
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| 50MG | ¥8505 | 有现货 |
|
| 100MG | ¥11502 | 有现货 |
|
| 500MG | ¥23085 | 有现货 |
|
| 1G | 获取报价 | 有现货 |
|
生物学信息
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产品名称Drinabant
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注意事项本公司产品仅用于科研实验,不得用于人体或动物的临床与诊断
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产品简述Drinabant 是一种口服活性 CB1 受体拮抗剂。 Drinabant 抑制激动剂刺激的钙信号,对 hCB1-R 和 rCB1-R 的 IC50 值分别为 25 nM 和 10 nM,对 hCB2-R 无效。
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产品描述Drinabant is an orally active CB1 receptor antagonist. Drinabant inhibits the agonist-stimulated calcium signal with IC50 values of 25 nM and 10 nM for the hCB1-R and rCB1-R, respectively, and is ineffective for the hCB2-R.(In Vivo):Drinabant (10 mg/kg orally once daily), combined with Olanzapine attenuates body weight gain, diminishing the enhanced food intake while maintaining increased energy expenditure and decreased motility. Drinabant (1, 3, and 10 mg/kg ip), reverses abnormally persistent LI induced by MK-801 or neonatal nitric oxide synthase inhibition in rodents, and improves both working and episodic memory.
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体外实验——
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体内实验AVE1625 (10 mg/kg orally once daily), combined with Olanzapine (HY-14541) attenuates body weight gain, diminishing the enhanced food intake while maintaining increased energy expenditure and decreased motility. AVE1625 (1, 3, and 10 mg/kg ip), reverses abnormally persistent LI induced by MK-801 (HY-15084B) or neonatal nitric oxide synthase inhibition in rodents, and improves both working and episodic memory. Animal Model:Rats.Dosage:30 mg/kg.Administration:Oral gavage, single dose.Result:Had free access to food during the preceding night (postprandial state) caused a pronounced reduction of food intake during the subsequent 10-12 h without differences intheir locomotor activity relative to that of the control group.Caused an increase in FFA and glycerol, indicating increased lipolysis from fat tissue.Immediately resulted in a pronounced increase in VCO2 and VO2, indicating increased oxidation of energetic substrates and increased TEE.Animal Model:Female Hanover Wistar rats weighing 225 ± 8.6 g.Dosage:10 mg/kg.Administration:Orally once daily.Result:Reduced their weight markedly within the first 3 days of treatment where upon animals maintained lower body weight, although they lost about 7.3 ± 1.3 g fat during the 12 days of treatment.
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同义词AVE-1625
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通路GPCR/G Protein
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靶点Cannabinoid Receptor
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受体TRPV1
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研究领域——
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适应症——
化学信息
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CAS Number358970-97-5
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分子量497.39
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分子式C23H20Cl2F2N2O2S
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纯度>98% (HPLC)
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溶解度——
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SMILESCS(N(C(C1)CN1C(c(cc1)ccc1Cl)c(cc1)ccc1Cl)c1cc(F)cc(F)c1)(=O)=OCS(N(C(C1)CN1C(c(cc1)ccc1Cl)c(cc1)ccc1Cl)c1cc(F)cc(F)c1)(=O)=O
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化学全称——
运输与储存
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储存条件(-20℃)
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运输条件With Ice Pack
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稳定性≥ 2 years
参考文献
1.Kym PR, Kort ME, Hutchins CW. Analgesic potential of TRPV1 antagonists. Biochem Pharmacol. 2009 Aug 1;78(3):211-6.
