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首页> 外文期刊>Journal of Medicinal Chemistry >Highly Potent First Examples of Dual Aromatase-Steroid Sulfatase Inhibitors based on a Biphenyl Template
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Highly Potent First Examples of Dual Aromatase-Steroid Sulfatase Inhibitors based on a Biphenyl Template

机译:基于联苯模板的双重芳香酶-类固醇硫酸酯酶抑制剂的高效实例

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Single agents against multiple drug targets are of increasing interest. Hormone-dependent breast cancer (HDBC) may be more effectively treated by dual inhibition of aromatase and steroid sulfatase (STS). The aromatase inhibitory pharmacophore was thus introduced into a known biphenyl STS inhibitor to give a series of novel dual aromatase-sulfatase inhibitors (DASIs). Several compounds are good aromatase or STS inhibitors and DASI 20 (IC50: aromatase, 2.0 nM; STS, 35 nM) and its chlorinated congener 23 (IC50: aromatase, 0.5 nM; STS, 5.5 nM)are examples that show exceptional dual potency in JEG-3 cells. Both biphenyls share a para-sulfamate-containing ring B and a ring A, which contains a triazol-1-ylmethyl meta to the biphenyl bridge and para to a nitrile. At 1 mg/kg po, 20 and 23 reduced plasma estradiol levels strongly and inhibited liver STS activity potently in vivo. 23 is nonestrogenic and potently inhibits carbonic anhydrase II (IC50 86 nM). A complex was crystallized and its structure was solved by X-ray crystallography. This class of DASI should encourage further development toward multitargeted therapeutic intervention in HDBC.
机译:针对多种药物靶标的单药越来越受到关注。通过双重抑制芳香化酶和类固醇硫酸酯酶(STS),可以更有效地治疗激素依赖性乳腺癌(HDBC)。因此,将芳香化酶抑制药效基团引入到已知的联苯STS抑制剂中,得到了一系列新型的双重芳香化酶-硫酸酯酶抑制剂(DASI)。几种化合物是良好的芳香酶或STS抑制剂,DASI 20(IC50:芳香酶,2.0 nM; STS,35 nM)及其氯化同源物23(IC50:芳香酶,0.5 nM; STS,5.5 nM)是显示出优异的双重功效的实例。 JEG-3细胞。两个联苯共有一个含对氨基磺酸酯的环B和一个环A,该环在联苯桥和腈上都含有一个三唑-1-基甲基间位。口服1 mg / kg时,20和23会强烈降低血浆雌二醇水平,并在体内有效抑制肝脏STS活性。 23是非雌激素的,可有效抑制碳酸酐酶II(IC50 86 nM)。使配合物结晶,并通过X射线晶体学解析其结构。此类DASI应该鼓励HDBC向多目标治疗干预的进一步发展。

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