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与普鲁卡因酰胺偶联的5-氨基水杨酸通过对核因子κB的加成抑制作用作为抗结肠炎互前药。

5-Aminosalicylic Acid Azo-Linked to Procainamide Acts as an Anticolitic Mutual Prodrug via Additive Inhibition of Nuclear Factor kappaB.

作者信息

Kim Wooseong, Nam Joon, Lee Sunyoung, Jeong Seongkeun, Jung Yunjin

机构信息

College of Pharmacy, Pusan National University , Busan 609-735, Republic of Korea.

出版信息

Mol Pharm. 2016 Jun 6;13(6):2126-35. doi: 10.1021/acs.molpharmaceut.6b00294. Epub 2016 May 5.

DOI:10.1021/acs.molpharmaceut.6b00294
PMID:27112518
Abstract

To improve the anticolitic efficacy of 5-aminosalicylic acid (5-ASA), a colon-specific mutual prodrug of 5-ASA was designed. 5-ASA was coupled to procainamide (PA), a local anesthetic, via an azo bond to prepare 5-(4-{[2-(diethylamino)ethyl]carbamoyl}phenylazo)salicylic acid (5-ASA-azo-PA). 5-ASA-azo-PA was cleaved to 5-ASA and PA up to about 76% at 10 h in the cecal contents while remaining stable in the small intestinal contents. Oral gavage of 5-ASA-azo-PA and sulfasalazine, a colon-specific prodrug currently used in clinic, to rats showed similar efficiency in delivery of 5-ASA to the large intestine, and PA was not detectable in the blood after 5-ASA-azo-PA administration. Oral gavage of 5-ASA-azo-PA alleviated 2,4,6-trinitrobenzenesulfonic acid-induced rat colitis. Moreover, combined intracolonic treatment with 5-ASA and PA elicited an additive ameliorative effect. Furthermore, combined treatment with 5-ASA and PA additively inhibited nuclear factor-kappaB (NFκB) activity in human colon carcinoma cells and inflamed colonic tissues. Finally, 5-ASA-azo-PA administered orally was able to reduce inflammatory mediators, NFκB target gene products, in the inflamed colon. 5-ASA-azo-PA may be a colon-specific mutual prodrug acting against colitis, and the mutual anticolitic effects occurred at least partly through the cooperative inhibition of NFκB activity.

摘要

为提高5-氨基水杨酸(5-ASA)的抗结肠炎疗效,设计了一种5-ASA的结肠特异性互作前药。5-ASA通过偶氮键与局部麻醉药普鲁卡因酰胺(PA)偶联,制备5-(4-{[2-(二乙氨基)乙基]氨基甲酰基}苯基偶氮)水杨酸(5-ASA-偶氮-PA)。5-ASA-偶氮-PA在盲肠内容物中10小时内可裂解为5-ASA和PA,裂解率高达约76%,而在小肠内容物中保持稳定。对大鼠口服灌胃5-ASA-偶氮-PA和柳氮磺胺吡啶(一种目前临床使用的结肠特异性前药),结果显示二者在将5-ASA递送至大肠方面效率相似,且给予5-ASA-偶氮-PA后血液中未检测到PA。口服灌胃5-ASA-偶氮-PA可减轻2,4,6-三硝基苯磺酸诱导的大鼠结肠炎。此外,5-ASA和PA联合结肠内治疗产生相加的改善作用。此外,5-ASA和PA联合治疗可相加抑制人结肠癌细胞和炎症结肠组织中的核因子-κB(NFκB)活性。最后,口服给予的5-ASA-偶氮-PA能够减少炎症结肠中的炎症介质,即NFκB靶基因产物。5-ASA-偶氮-PA可能是一种作用于结肠炎的结肠特异性互作前药,其相互抗结肠炎作用至少部分是通过协同抑制NFκB活性实现的。

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