首页> 外文期刊>Journal of enzyme inhibition and medicinal chemistry. >Some 3-(4-aminophenyl)pyrrolidine-2,5-diones as all-trans-retinoic acid metabolising enzyme inhibitors (RAMBAs).
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Some 3-(4-aminophenyl)pyrrolidine-2,5-diones as all-trans-retinoic acid metabolising enzyme inhibitors (RAMBAs).

机译:一些3-(4-氨基苯基)吡咯烷-2,5-二酮类化合物是全反式维甲酸代谢酶抑制剂(RAMBAs)。

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摘要

A series of (+/-)-3-(4-aminophenyl) pyrrolidin-2,5-diones substituted in the 1-, 3- or 1,3-position with an aryl or long chain alkyl function are weak inhibitors of the metabolism of all-trans retinoic acid (RA) by rat liver microsomes (68-75% inhibition) compared with ketoconazole (85%). Further studies with the 1-cyclohexyl analogue (1) (IC50 = 98.8 microM, ketoconazole, 22.15 microM) showed that it was not stereoselective in its inhibition. (+/-)-(1) was not an inhibitor of pig brain microsomal enzyme (ketoconazole, IC50 = 20.9 microM), had little effect on human liver microsomal enzyme (19.3%, ketoconazole, 81.6%) or human placental microsomal enzyme (9.8%, ketoconazole 73.9%) but was a weak inhibitor of human and rat skin homogenates (52.6% and IC50 = 211.6 microM respectively; ketoconazole, 38.8% and 85.95 microM). In RA-induced cell cultures of human male genital fibroblasts and HaCat cells, (+/-)-(1) was a weak inhibitor (c. 53% at 200 microM) whereas ketoconazole showed high potency (c. 65% at0.625 microM and 0.25 microM respectively). The nature of the induced target enzyme is discussed.
机译:在1-,3-或1,3-位上被芳基或长链烷基官能团取代的一系列(+/-)-3-(4-氨基苯基)吡咯烷-2,5-二酮是弱抑制剂与酮康唑(85%)相比,大鼠肝脏微粒体的全反式维甲酸(RA)代谢(抑制68-75%)。对1-环己基类似物(1)(IC50 = 98.8 microM,酮康唑,22.15 microM)的进一步研究表明,其抑制作用不是立体选择性的。 (+/-)-(1)不是猪脑微粒体酶的抑制剂(酮康唑,IC50 = 20.9 microM),对人肝微粒体酶(19.3%,酮康唑,81.6%)或人胎盘微粒体酶(酮康唑为9.8%,酮康唑为73.9%),但它是人和大鼠皮肤匀浆的弱抑制剂(分别为52.6%和IC50 = 211.6 microM;酮康唑为38.8%和85.95 microM)。在RA诱导的人类雄性生殖纤维细胞和HaCat细胞的细胞培养物中,(+/-)-(1)是弱抑制剂(在200 microM时约为53%),而酮康唑则显示出高效力(在0.625时约为65%)。 microM和0.25 microM)。讨论了诱导的靶酶的性质。

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