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Design, synthesis and evaluation of novel 16-imidazolyl substituted steroidal derivatives possessing potent diversified pharmacological properties.

机译:具有强大的多种药理特性的新型16-咪唑基取代的甾族衍生物的设计,合成和评估。

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摘要

As a part of our investigations into the structural-activity relationship studies of a novel class of medicinally active 16-substituted steroids, several new 16-imidazolyl substituted steroidal derivatives have been synthesized and pharmacologically evaluated in the current study. The new steroidal analogues 5, 6, 8, 9, 11 and 12 exhibited moderate cytotoxic effects in sixty cancer cell lines derived from nine cancers types. The imidazolyl substituted steroidal derivatives 6 (DPJ-RG-1241) and 7 (RB-401) were obtained as the powerful inhibitors of aromatase with IC50=0.18 μM and IC50=0.168 μM, respectively, approximately 1.2 and 1.4 times more potent in comparison to standard drug exemestane. The bis-quaternary steroids 13 and 14 displayed potent skeletal muscle relaxant properties. An affinity constant of 0.007 μM was observed for compound 14 on frog rectus abdominis muscle preparation and 13 displayed a very high anticholinesterase activity K(i)=25 nM, approximately 115-fold higher in comparison to standard drug galanthamine (K(i)=2.9 μM).
机译:作为我们对一类新型的具有医学活性的16-取代的类固醇的结构-活性关系研究的一部分,在本研究中已经合成了几种新的16-咪唑基取代的类固醇衍生物,并对其药理学进行了评估。新的类固醇类似物5、6、8、9、11和12在源自九种癌症类型的60个癌细胞系中表现出中等的细胞毒性作用。获得了咪唑基取代的甾体衍生物6(DPJ-RG-1241)和7(RB-401)作为芳香化酶的强大抑制剂,其IC50分别为0.150μM和IC50 = 0.168μM,分别是其有效价的1.2倍和1.4倍到标准药物依西美坦。双季类固醇13和14具有强效的骨骼肌松弛特性。观察到化合物14在蛙直肌腹部肌肉上的亲和常数为0.007μM,而13则显示出很高的抗胆碱酯酶活性K(i)= 25 nM,与标准药物加兰他敏(K(i)= 2.9μM)。

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