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A study of factors influencing drug disposition in chronic liver disease, using the model drug (+)-propranolol.

机译:使用模型药物(+)-心得安对慢性肝病中药物处置的影响因素进行研究。

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摘要

The pharmacokinetics, following i.v. administration of (+)-propranolol (40 mg) have been compared to in vitro measurement of protein binding and biochemical parameters of liver function in six normal subjects and twenty patients with stable chronic liver disease. The clearance of (+)-propranolol decreased with evidence of increasing severity of impairment of liver function correlating significantly with a fall in serum albumin, a rise in bilirubin and a prolongation in prothrombin index. The clearance of (+)-propranolol correlated with and was numerically similar to the clearance of indocyanine green in normal subjects and also in patients with chronic liver disease. Protein binding was decreased in chronic liver disease, but this change was not related to changes in plasma proteins. In normal subjects and patients without ascites the volume of distribution increased with decreases in protein binding. Ascites was associated with a further increase in the volume of distribution. The considerable variation in half-life largely depends on changes in liver blood flow, the degree of protein binding and the plasma protein pool size.
机译:i.v.之后的药代动力学已将(+)-普萘洛尔(40 mg)的给药与6位正常受试者和20位稳定的慢性肝病患者的肝功能蛋白质结合和生化参数的体外测量进行了比较。 (+)-普萘洛尔的清除率降低,肝功能损害严重程度增加的证据与血清白蛋白下降,胆红素升高和凝血酶原指数延长显着相关。 (+)-普萘洛尔的清除率与正常受试者和慢性肝病患者的吲哚菁绿的清除率相关,并在数值上相似。在慢性肝病中蛋白质结合减少,但是这种变化与血浆蛋白质的变化无关。在正常受试者和无腹水的患者中,分布体积随着蛋白质结合的减少而增加。腹水与分布量的进一步增加有关。半衰期的显着变化在很大程度上取决于肝脏血流量,蛋白质结合程度和血浆蛋白质库大小的变化。

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