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复方磺胺甲恶唑的临床药代动力学。

Clinical pharmacokinetics of co-trimazine.

作者信息

Bergan T, Ortengren B, Westerlund D

出版信息

Clin Pharmacokinet. 1986 Sep-Oct;11(5):372-86. doi: 10.2165/00003088-198611050-00003.

Abstract

The clinical pharmacokinetics of co-trimazine (trimethoprim plus sulphadiazine) are reviewed and compared with those of co-trimoxazole (trimethoprim plus sulphamethoxazole). Both combination drugs have similar serum half-life values in persons with normal renal function (half-life of 8 to 12 hours), but the sulphamethoxazole metabolites are retained more than trimethoprim in reduced renal function. Sulphadiazine is less metabolised and the total sulphonamide load of therapeutic doses of co-trimazine is therefore less than for co-trimoxazole. Both co-trimazine and co-trimoxazole have high bioavailability. A suspension of co-trimazine gives serum concentrations comparable with those of tablets. The extravascular penetration of the co-trimazine components is reflected by the total area under the lymph concentration curve in comparison with serum. This measure shows a penetration into peripheral human lymph of 68% for sulphadiazine and 59% for trimethoprim. The proportions eliminated in urine are about 55% for sulphadiazine, 30% for its acetylated metabolite and 75% for trimethoprim. In comparison, for co-trimoxazole, the proportion of sulphamethoxazole eliminated in urine is 15%, that of the acetylated derivative 47%, and that of trimethoprim is also 75%. Urine concentrations of both combinations have similar bioactivity against urinary pathogens after 500 mg of co-trimazine and 960 mg of co-trimoxazole.

摘要

本文综述了复方磺胺嘧啶(甲氧苄啶加磺胺嘧啶)的临床药代动力学,并与复方新诺明(甲氧苄啶加磺胺甲恶唑)进行了比较。在肾功能正常的人群中,这两种复方药物的血清半衰期值相似(半衰期为8至12小时),但在肾功能减退时,磺胺甲恶唑的代谢产物比甲氧苄啶保留得更多。磺胺嘧啶的代谢较少,因此治疗剂量的复方磺胺嘧啶的总磺胺负荷低于复方新诺明。复方磺胺嘧啶和复方新诺明都具有高生物利用度。复方磺胺嘧啶混悬液的血清浓度与片剂相当。与血清相比,复方磺胺嘧啶成分的血管外渗透可通过淋巴浓度曲线下的总面积反映出来。该指标显示磺胺嘧啶在外周人体淋巴中的渗透率为68%,甲氧苄啶为59%。磺胺嘧啶经尿液排出的比例约为55%,其乙酰化代谢产物为30%,甲氧苄啶为75%。相比之下,对于复方新诺明,磺胺甲恶唑经尿液排出的比例为15%,其乙酰化衍生物为47%,甲氧苄啶也为75%。服用500mg复方磺胺嘧啶和960mg复方新诺明后,两种复方药物的尿液浓度对尿路病原体具有相似的生物活性。

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