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21102-95-4 BMY 7378 DIHYDROCHLORIDE;8-(2-[4-(2-METHOXYPHENYL)-1-PIPERAZINYL]ETHYL)-8-AZASPIRO(4,5)DECANE-7,9-DIONE DIHYDROCHLORIDE

产品信息
  • BMY-7378
    分子式:C22H31N3O3.2HCl
    分子量:458.42
    产品描述
    BMY 7378是多

    靶点

    YZ剂,作用于α2C-adrenoceptor和α1D-adrenoceptor,pKi分别为6.54 和8.2,且作为混合型5-HT1A受体激动剂和拮抗剂,pKi为8.3。

    靶点

    α2C-adrenoceptorα1D-adrenoceptor IC506.54 (pKi)8.2 (pKi)
    体外研究
    BMY 7378 shows 10-fold selectivity for α2C-adrenoceptors over other α2-adrenoceptors with pKi of 6.54.BMY 7378 is selective for the α1D-adrenoceptor subtype (PKi: hamster α1b-adrenoceptor 6.2, human α1b-adrenoceptor 7.2; bovine α1c-adrenoceptor 6.1, human α1c-adrenoceptor 6.6; rat α1d-adrenoceptor 8.2, human α1d-adrenoceptor 9.4.BMY 7378 at concentration of 1 nM to 30 nM elicits inhibitory effects in a concentration-dependent manner in the rat dorsal raphe nucleus.
    体内研究
    BMY 7378 (pA2 of 8.67) is approximately 100 times more potent than yohimbine (pA2 of 6.62) against contractions to noradrenaline in rat aorta. BMY 7378 (pA2 of 6.48) is approximately 10 times less potent than yohimbine (pA2 of 7.56) at antagonizing the contractile response to noradrenaline in human saphenous vein (α2C-adrenoceptor).BMY 7378 dose dependently (0.25-5 mg/kg s.c.) reduces the undetectable levels forepaw treading and head weaving induced by 8-OH-DPAT (0.75 mg/kg s.c.) in rats. BMY 7378 causes a marked and dose-dependent (0.01-1.0 mg/kg s.c.) decrease of 5-HT release in ventral hippocampus of the anaesthetized rat as detected by brain microdialysis in rats.溶解性DMSO 92 mg/mL,水 92 mg/mL,乙醇 20 mg/mL
    稳定性
    2年 -20°C粉状,6月-80°C溶于DMSO
    特征
    温馨提示:不可用于临床ZL。
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