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呋喃妥因的药代动力学及其相关生物利用度。

The pharmacokinetics of nitrofurantoin and its related bioavailability.

作者信息

Conklin J D

出版信息

Antibiot Chemother (1971). 1978;25:233-52. doi: 10.1159/000401065.

Abstract

Nitrofurantoin is a urinary tract antibacterial agent whose clinical effectiveness depends on the high urinary drug levels encountered during therapeutic drug dosage. Under these conditions, only low blood drug concentrations are usually found. On the basis of urinary nitrofurantoin excretion determined after oral and intravenous drug administration, orally administered nitrofurantoin in a suitable dosage form is well absorbed. In vitro testing does not accurately reflect nitrofurantoin bioavailability, which is affected by formulation differences, drug particle size, and dosage form. Nitrofurantoin is readily absorbed and quickly distributed into most body fluids. It is rapidly excreted in large amounts in bile and urine. With the exception of the active drug secretion in the kidney tubule and biliary drug transport, nitrofurantoin transfer across body membranes occurs by diffusion. Nitrofurantoin has a short elimination half-life in whole blood or plasma. In conjunction with its rapid excretion by the primary routes, there is little evidence for any prolonged binding of nitrofurantoin to either plasma proteins or tissues. The first-order kinetics involved in nitrofurantoin absorption and elimination is most appropriately described by a one-compartment open model. Biliary and urinary excretion of unchanged nitrofurantoin and enzymatic degradation are the primary means of elimination.

摘要

呋喃妥因是一种尿路抗菌剂,其临床疗效取决于治疗药物剂量时尿液中的高药物水平。在这些情况下,通常仅发现低血药浓度。根据口服和静脉给药后测定的呋喃妥因尿排泄情况,合适剂型的口服呋喃妥因吸收良好。体外试验不能准确反映呋喃妥因的生物利用度,其受制剂差异、药物粒径和剂型的影响。呋喃妥因易于吸收并迅速分布到大多数体液中。它在胆汁和尿液中大量迅速排泄。除了肾小管中的活性药物分泌和胆汁药物转运外,呋喃妥因通过扩散穿过身体膜。呋喃妥因在全血或血浆中的消除半衰期较短。结合其主要途径的快速排泄,几乎没有证据表明呋喃妥因与血浆蛋白或组织有任何长时间的结合。呋喃妥因吸收和消除所涉及的一级动力学最适合用单室开放模型来描述。未改变的呋喃妥因的胆汁和尿液排泄以及酶促降解是主要的消除方式。

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