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一项确定柳氮磺胺吡啶活性治疗部分的实验。

An experiment to determine the active therapeutic moiety of sulphasalazine.

作者信息

Azad Khan A K, Piris J, Truelove S C

出版信息

Lancet. 1977 Oct 29;2(8044):892-5. doi: 10.1016/s0140-6736(77)90831-5.

Abstract

Sulphasalazine (S.A.S.P.) is of proven value in the treatment of ulcerative colitis, but its mode of action is unknown. When it is taken by mouth, nearly all the dose reaches the colon intact, where it is split by bacteria into sulphapyridine (S.P.) and 5-aminosalicylic acid (5-A.S.A.). An experiment was devised to determine whether the therapeutic property of S.A.S.P. is a function of the parent molecule or of these two principal metabolites. Retention enemas of S.A.S.P., S.P., and 5-A.S.A. were administered to volunteer patients with sigmoidoscopic evidence of active ulcerative colitis. The experiment was conducted as a blind controlled therapeutic trial, each patient having one of the test enemas daily for two weeks. Pronounced histological improvement was observed in approximately 30% of the patients receiving S.A.S.P. or 5-A.S.A., and in only 5% of those receiving S.P. It is concluded that the active therapeutic moiety of S.A.S.P. IS 5-A.S.A. and that the S.P. functions as a carrier ensuring that the 5-A.S.A. is liberated within the colon.

摘要

柳氮磺胺吡啶(S.A.S.P.)在治疗溃疡性结肠炎方面已被证明具有疗效,但其作用方式尚不清楚。口服时,几乎所有剂量的药物都完整地到达结肠,在那里被细菌分解为磺胺吡啶(S.P.)和5-氨基水杨酸(5-A.S.A.)。设计了一项实验来确定S.A.S.P.的治疗特性是母体分子的作用还是这两种主要代谢产物的作用。对有乙状结肠镜检查显示为活动性溃疡性结肠炎的志愿者患者给予S.A.S.P.、S.P.和5-A.S.A.保留灌肠剂。该实验作为一项盲法对照治疗试验进行,每位患者每天接受一种试验灌肠剂,持续两周。在接受S.A.S.P.或5-A.S.A.的患者中,约30%观察到明显的组织学改善,而接受S.P.的患者中只有5%观察到明显改善。得出的结论是,S.A.S.P.的活性治疗部分是5-A.S.A.,而S.P.起到载体的作用,确保5-A.S.A.在结肠内释放。

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