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回肠末端和结肠:5-氨基水杨酸释放的靶向部位。

Distal ileum and colon: targeted sites for 5-ASA release.

作者信息

Devane J, Mulligan S, Martin M

机构信息

Elan Corporation plc. Athlone, Ireland.

出版信息

Eur J Drug Metab Pharmacokinet. 1991;Spec No 3:300-3.

PMID:1820897
Abstract

Sulphasalazine, used in the treatment of ulcerative colitis, is cleaved in the colon by the metabolic action of colonic bacteria on the diazo bond to release 5-Aminosalicylic acid (5-ASA) and sulpharidine. Whilst the former has been demonstrated to be active moiety, the latter is reputed to be responsible for toxicity associated with sulphasalazine therapy. A new multi-particulate formulation of 5-ASA has been designed (Asalan) to achieve targeted release of the drug in both the distal small intestine and colon and hence may be beneficial in the treatment of not only Ulcerative Colitis but also Crohn's disease. An imaging study was performed with beads formulated with barium sulphate using the same procedure employed to prepare 5-ASA beads. This study suggested 5-ASA capsule disintegration and bead dispersal in both the distal ileum and colon. This targetting was confirmed in two further in vivo studies using the 5-ASA formulation itself. In the first study comparison of plasma ASA levels following treatment with sulphasalazine treatment confirmed that 5-ASA release was occurring proximal to the colon. Despite this earlier release, the percentage of administered dose that was unabsorbed (dose-urinary recovery) was approximately 90%. In a second study a comparison was made with a single unit tablet of 5-ASA. A greater consistency and accuracy of targetting, as revealed by the appearance of plasma ASA levels, was confirmed for the capsule formulation. These separate studies were undertaken to evaluate the in vivo intestinal release characteristics of this new 5-ASA formulation in healthy volunteers.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

用于治疗溃疡性结肠炎的柳氮磺胺吡啶,在结肠中通过结肠细菌对重氮键的代谢作用而裂解,释放出5-氨基水杨酸(5-ASA)和磺胺吡啶。虽然前者已被证明是活性部分,但后者被认为是与柳氮磺胺吡啶治疗相关毒性的原因。一种新的5-ASA多颗粒制剂(Asalan)已被设计出来,以实现药物在远端小肠和结肠中的靶向释放,因此不仅可能对溃疡性结肠炎的治疗有益,而且对克罗恩病的治疗也有益。使用制备5-ASA微珠的相同程序,对用硫酸钡配制的微珠进行了成像研究。这项研究表明5-ASA胶囊在回肠末端和结肠中均发生崩解和微珠分散。在另外两项使用5-ASA制剂本身的体内研究中证实了这种靶向性。在第一项研究中,比较柳氮磺胺吡啶治疗后血浆ASA水平,证实5-ASA在结肠近端释放。尽管有这种早期释放,但未吸收的给药剂量百分比(剂量-尿液回收率)约为90%。在第二项研究中,将其与5-ASA单单位片剂进行了比较。胶囊制剂在血浆ASA水平表现上显示出更高的靶向一致性和准确性。进行这些单独的研究是为了评估这种新的5-ASA制剂在健康志愿者体内的肠道释放特性。(摘要截短于250字)

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