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A Prodrug Approach Toward Cancer-Related Carbonic Anhydrase Inhibition

机译:抑制癌症相关碳酸酐酶的前药方法

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摘要

The selective inhibition of cancer-associated human carbonic anhydrase (CA) enzymes, specifically CA IX and XII, has been validated as a mechanistically novel approach toward personalized cancer management. Herein we report the design and synthesis of a panel of 24 novel glycoconjugate primary sulfonamides that bind to the extracellular catalytic domain of CA IX and XII. These compounds were synthesized from variably acylated glycopyranosyl azides and either 3- or 4-ethynyl benzene sulfonamide using Cu(I)-catalyzed azide alkyne cycloaddition (CuAAC). The CA enzyme inhibition profile for all compounds was determined, while in vitro metabolic stability, plasma stability, and plasma protein binding for a representative set of compounds was measured. Our findings demonstrate the influence of the differing acyl groups on these key biopharmaceutical properties, confirming that acyl group protected carbohydrate-based sulfonamides have potential as prodrugs for selectively targeting the extracellular cancer-associated CA enzymes. (1) Alterio, V.; Di Fiore, A.; D'Ambrosio, K.; Supuran, C. T.; De Simone, G. Multiple binding modes of inhibitors to carbonic anhydrases: how to design specific drugs targeting 15 different isoforms? Chem. Rev. 2012, 112, 4421?4468.
机译:对癌症相关的人类碳酸酐酶(CA)酶(特别是CA IX和XII)的选择性抑制已被验证为针对个性化癌症管理的机械新颖方法。在本文中,我们报道了一组与CA IX和XII的胞外催化结构域结合的24种新型糖缀合物伯磺酰胺的设计和合成。这些化合物是使用Cu(I)催化的叠氮化物炔烃环加成反应(CuAAC)由可变酰基化的吡喃葡萄糖基叠氮化物和3-或4-乙炔基苯磺酰胺合成的。确定了所有化合物的CA酶抑制曲线,同时测量了一组代表性化合物的体外代谢稳定性,血浆稳定性和血浆蛋白结合。我们的发现证明了不同酰基对这些关键生物药物特性的影响,证实了酰基保护的基于碳水化合物的磺酰胺具有作为选择性靶向细胞外癌相关CA酶的前药的潜力。 (1)Alterio,V。 Di Fiore,A .; D'Ambrosio,K。 Supuran,C. T .; De Simone,G.抑制剂与碳酸酐酶的多种结合方式:如何设计针对15种不同亚型的特定药物?化学修订版2012,112,4421?4468。

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