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托美丁钠的前体药物托美丁甘氨酰胺(McN-4366)对大鼠佐剂性关节炎的影响。

Effect of tolmetin glycine amide (McN-4366), a prodrug of tolmetin sodium, on adjuvant arthritis in the rat.

作者信息

Persico F J, Pritchard J F, Fisher M C, Yorgey K, Wong S, Carson J

机构信息

Department of Biological Research, McNeil Pharmaceutical, Spring House, Pennsylvania.

出版信息

J Pharmacol Exp Ther. 1988 Dec;247(3):889-96.

PMID:3204521
Abstract

The glycine amide of tolmetin sodium (TGA) functions as a prodrug and was demonstrated to be more potent than the parent compound as an inhibitor of developing and established adjuvant arthritis in the female Lewis rat. In contrast, the glycine amide of indomethacin was less potent than indomethacin. The superiority of TGA relative to tolmetin sodium in alleviating this condition was demonstrated by inhibition of paw swelling and reduction of the degenerative bone changes that are associated with the progression of this chronic animal model of rheumatoid arthritis in humans. These properties were not evident when equimolar mixtures of tolmetin sodium and glycine were administered concurrently. Pharmacokinetic analyses revealed that TGA was absorbed completely and hydrolyzed to tolmetin in the female adjuvant arthritic rat. The combined effects of absorption, distribution and hydrolysis of TGA produced lower peak plasma tolmetin levels than an equivalent dose of tolmetin sodium, but plasma concentrations were sustained for a longer period of time contributing to an apparent increase in potency. Furthermore, TGA displayed a decreased propensity to cause gastrointestinal irritation compared to tolmetin sodium. Several additional amino acid amides of tolmetin were similar to the glycine amide in exhibiting increased potency and reduced gastrointestinal toxicity in comparison to equivalent doses of tolmetin sodium.

摘要

托美丁钠的甘氨酰胺(TGA)起前药的作用,并且已证明其作为雌性Lewis大鼠中正在发展和已形成的佐剂性关节炎的抑制剂,比母体化合物更有效。相比之下,吲哚美辛的甘氨酰胺比吲哚美辛的效力低。通过抑制爪肿胀以及减少与人类类风湿性关节炎这种慢性动物模型进展相关的退行性骨变化,证明了TGA相对于托美丁钠在缓解这种病症方面的优越性。当同时给予托美丁钠和甘氨酸的等摩尔混合物时,这些特性并不明显。药代动力学分析表明,TGA在雌性佐剂性关节炎大鼠中被完全吸收并水解为托美丁。TGA的吸收、分布和水解的综合作用产生的血浆托美丁峰值水平低于等剂量的托美丁钠,但血浆浓度维持的时间更长,这导致效力明显增加。此外,与托美丁钠相比,TGA引起胃肠道刺激的倾向降低。与等剂量的托美丁钠相比,托美丁的几种其他氨基酸酰胺在表现出效力增加和胃肠道毒性降低方面与甘氨酰胺相似。

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