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首页> 外文期刊>Bioorganic and medicinal chemistry >A novel library of saccharin and acesulfame derivatives as potent and selective inhibitors of carbonic anhydrase IX and XII isoforms
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A novel library of saccharin and acesulfame derivatives as potent and selective inhibitors of carbonic anhydrase IX and XII isoforms

机译:一种新型糖精和乙酰磺胺衍生物库,作为碳酸酐酶IX和XII同种型的有效和选择性抑制剂

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摘要

Small libraries of N-substituted saccharin and N-/O-substituted acesulfame derivatives were synthesized and tested as atypical and selective inhibitors of four different isoforms of human carbonic anhydrase (hCA I, II, IX and XII, EC 4.2.1.1). Most of them inhibited hCA XII in the low nanomolar range, hCA IX with K(I)s ranging between 19 and 2482 nM, whereas they were poorly active against hCA II (K(I)s > 10 mu M) and hCA I (K(I)s ranging between 318 nM and 50 mu M). Since hCA I and II are ubiquitous off-target isoforms, whereas the cancer-related isoforms hCA IX and XII were recently validated as drug targets, these results represent an encouraging achievement in the development of new anticancer candidates. Moreover, the lack of a classical zinc binding group in the structure of these inhibitors opens innovative, yet unexplored scenarios for different mechanisms of inhibition that could explain the high inhibitory selectivity. A computational approach has been carried out to further rationalize the biological data and to characterize the binding mode of some of these inhibitors. (C) 2016 Elsevier Ltd. All rights reserved.
机译:合成了N-取代的糖精和N- / O-取代的乙酰磺胺衍生物的小文库,并作为非典型和选择性抑制剂,其四种不同同种型人碳酸酐酶(HCA I,II,IX和XII,EC 4.2.1.1)。它们中的大多数抑制了低纳米摩尔范围内的HCA XII,HCA IX与K(i)的k(i)在19和2482nm之间的范围内,而它们对HCA II有效(K(i)S>10μm)和HCA I( K(i)在318nm和50 mu m之间的范围。由于HCA I和II是无处不在的偏离目标同种型,而癌症相关的同种型HCA IX和XII最近被验证为药物目标,这些结果代表了新的抗癌候选人的发展中的令人鼓舞的成就。此外,对于这些抑制剂的结构中缺乏经典的锌结合组开启了可用于不同抑制机制的创新性,但无法解释高抑制选择性的机制。已经进行了计算方法以进一步合理地利用生物数据并表征一些这些抑制剂的结合模式。 (c)2016 Elsevier Ltd.保留所有权利。

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