(S)-SLV 319
| 规格 | 价格 | 货期 | 数量 |
|---|---|---|---|
| 1mg | ¥1570.00 | 现货 | |
| 5mg | ¥4712.00 | 现货 | |
| 10mg | ¥7095.00 | 现货 |
特色产品
- 用于免疫印迹和质谱分析等后续操作
- 适用于30 KDa-130 KDa大小的蛋白
- 可将信号灵敏度提高100倍
- 同时保持稳定的特异性和分辨率
- 提供更高的转录效率并抑制免疫激活
- 使用5-moUTP和Cy5-utp修饰
产品描述
Ki: 7.8 and 7,9 nM for CB1 and peripheral cannabinoid (CB2), respectively
(S)-SLV 319 is a CB1 receptor antagonist.
It has been reported that central cannabinoid (CB1) receptor antagonists may have potential in the treatment of a variety of diseases including cognitive disorders, neuro-inflammatory disorders, obesity, septic shock, psychosis, addiction, as well as gastrointestinal disorders.
In vitro: Previous study found that (S)-SLV 319 was a potent and selective CB1 receptor antagonist with Ki values of 7.8 and 7,9 nM for CB1 and CB2, respectively. In addition, (S)-SLV 319 was found to be less lipophilic and thus more water soluble than other previously identified ligands of CB1 receptor [1].
In vivo: Previous animal study showed that in rats exposed to an ambient temperature of 22°c, a moderate dose of LPS at 25 - 100 μg/kg could induce a fall in body temperature. Such response was not affected by desensitization of intra-abdominal TRPV1 receptors with resiniferatoxin at 20 μg/kg, by systemic TRPV1 antagonism with capsazepine at 40 mg/kg, or by systemic CB2 receptor antagonism with SR144528 at 1.4 mg/kg. In contrast, CB1 receptor antagonism by SLV319 at 15 mg/kg or rimonabant at 4.6 mg/kg was able to block LPS caused hypothermia [2].
Clinical trial: So far, no clinical study has been conducted.
References:
[1] J. H. M. Lange, H. H. van Stuivenberg, W. Veerman, et al. Novel 3,4-diarylpyrazolines as potent cannabinoid CB1 receptor antagonists with lower lipophilicity. Bioorganic & Medicinal Chemistry Letters 15, 4794-4798 (2005).
[2] Steiner AA et al. The hypothermic response to bacterial lipopolysaccharide critically depends on brain CB1, but not CB2 or TRPV1, receptors. J Physiol. 2011 May 1;589(Pt 9):2415-31.
产品性质
| 物理外观 | A crystalline solid |
| CAS号 | 464213-10-3 |
| 分子式 | C23H20Cl2N4O2S |
| 分子量 | 487.4 |
| 小分子别名 | Ibipinabant |
| 化学名称 | 3-(4-chlorophenyl)-N-[(4-chlorophenyl)sulfonyl]-4,5-dihydro-N'-methyl-4S-phenyl-1H-pyrazole-1-carboximidamide |
| 溶解度 | ≤30mg/ml in ethanol;30mg/ml in DMSO;30mg/ml in dimethyl formamide |
| SMILES | C/N=C(\NS(c(cc1)ccc1Cl)(=O)=O)/N(C[C@@H]1c2ccccc2)N=C1c(cc1)ccc1Cl |
| 存储条件 | -20°C |
| 运输条件 | 蓝冰 |
产品应用 (实验数据来自文献,APExBIO并未验证,仅供参考)
IC50和靶点
| 生物活性描述 | 伊必那班(SLV319)是一种强效、选择性和口服活性的大麻素 CB1 受体拮抗剂,其 K i 为 7.8 nM,对 CB1 的选择性是 CB2 的 1000 倍(K i =7943 nM)。它被用于肥胖症和糖尿病的研究。 |



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