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碳酸酐酶抑制剂:用同时含有苯磺酰胺部分的亚氨基二乙酸羧酸盐/异羟肟酸抑制胞质/肿瘤相关同工型I、II和IX。

Carbonic anhydrase inhibitors: inhibition of cytosolic/tumor-associated isoforms I, II, and IX with iminodiacetic carboxylates/hydroxamates also incorporating benzenesulfonamide moieties.

作者信息

Santos M Amelia, Marques Sergio, Vullo Daniela, Innocenti Alessio, Scozzafava Andrea, Supuran Claudiu T

机构信息

Centro de Química Estrutural, Instituto Superior Técnico, Rua Rovisco Pais 1, 1049-001 Lisbon, Portugal.

出版信息

Bioorg Med Chem Lett. 2007 Mar 15;17(6):1538-43. doi: 10.1016/j.bmcl.2006.12.107. Epub 2007 Jan 8.

Abstract

The synthesis of a new class of sulfonamide carbonic anhydrase (CA, EC 4.2.1.1) inhibitors (CAIs), also possessing carboxylate/hydroxamate moieties in their molecule, is reported. These compounds may act on dual antitumor targets, the tumor-associated CA isozymes (CA IX) and some matrix metalloproteinases (MMPs). The compounds were prepared by an original method starting from iminodiacetic acid, and assayed as inhibitors of three isozymes, hCA I, II (cytosolic), and IX (transmembrane). The new derivatives showed weak inhibitory activity against isozyme I (K(I)s in the range of 95-8300 nM), were excellent to moderate CA II inhibitors (K(I)s in the range of 8.4-65 nM), and very good and selective CA IX inhibitors (K(I)s in the range of 3.8-26 nM). The primary sulfonamide moiety is a better zinc-binding group in the design of CAIs as compared to the carboxylate/hydroxamate one, but the presence of hydroxamate functionalities in the molecule of CAIs leads to selectivity for the tumor-associated isozyme IX over the ubiquitous, cytosolic isoform II.

摘要

报道了一类新型磺酰胺类碳酸酐酶(CA,EC 4.2.1.1)抑制剂(CAIs)的合成,其分子中还含有羧酸盐/异羟肟酸酯部分。这些化合物可能作用于双重抗肿瘤靶点,即肿瘤相关的CA同工酶(CA IX)和一些基质金属蛋白酶(MMPs)。这些化合物通过一种从亚氨基二乙酸开始的原始方法制备,并作为三种同工酶hCA I、II(胞质型)和IX(跨膜型)的抑制剂进行了测定。新衍生物对同工酶I显示出较弱的抑制活性(K(I)值在95 - 8300 nM范围内),是优秀至中等的CA II抑制剂(K(I)值在8.4 - 65 nM范围内),以及非常好且具有选择性的CA IX抑制剂(K(I)值在3.8 - 26 nM范围内)。与羧酸盐/异羟肟酸酯部分相比,在CAIs设计中,伯磺酰胺部分是更好的锌结合基团,但CAIs分子中异羟肟酸官能团的存在导致对肿瘤相关同工酶IX的选择性高于普遍存在的胞质型同工酶II。

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