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首页> 外文期刊>Bioorganic and Medicinal Chemistry Letters >Microbial hydroxylation and glycosylation of pentacyclic triterpenes as inhibitors on tissue factor procoagulant activity
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Microbial hydroxylation and glycosylation of pentacyclic triterpenes as inhibitors on tissue factor procoagulant activity

机译:五胞苷羟基化和戊基三萜胶剂作为组织因子促凝血活性的抑制剂

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摘要

To discover new inhibitors on tissue factor procoagulant activity, 20 pentacyclic triterpenes were semi-synthetized through microbial transformation and assayed on the model of human THP-1 cells stimulated by lipopolysaccharide. In the biotransformation two types of reactions were observed, regio-selective hydroxylation and glycosylation. The bioassay results showed that most of tested compounds were significant effective on this model and two of the biotransformation products 23-hydroxy-28-O-beta-o-glu-copyranosyl betulinic acid (3d) and 28-O-beta-u-glucopyranosyl oleanic acid (1a) exhibited most potential activities with the IC50 values of 0.028, 0.035 nM respectively. The preliminary structure and activity relationship analysis revealed that the aglycones with single free hydroxyl group on the skeleton (1, 1j) were less effective than that with more free hydroxyl groups (1d, 1f, 2), mono-glycosylation can significantly enhance their inhibitory effects. Our findings also provide some potential leading compounds for tissue factor-related diseases, such as cancer and cardiovascular diseases. (C) 2017 Elsevier Ltd. All rights reserved.
机译:为了发现组织因子促进活性的新抑制剂,通过微生物转化半合成20个五环三萜,并在脂多糖刺激的人THP-1细胞模型上测定。在生物转化中,观察到两种类型的反应,可选择羟基化和糖基化。生物测定结果表明,大多数经测试的化合物对该模型有效,两种生物转化产物23-羟基-28-O-β-O-Glu-Coderylylyl(3D)和28-O-Beta-U-有效葡萄糖醇烯酸(1A)显示出最多的潜在活动,分别为0.028,0.035nm的IC 50值。初步结构和活性关系分析显示,在骨架(1,1j)上具有单自由羟基的糖基比用更多的游离羟基(1d,1f,2),单糖基化可以显着增强它们的抑制性效果。我们的研究结果还为组织因子相关疾病提供了一些潜在的主要化合物,例如癌症和心血管疾病。 (c)2017 Elsevier Ltd.保留所有权利。

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