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新型β-肾上腺素能阻滞剂盐酸卡替洛尔(OPC - 1085)VIII的代谢命运。卡替洛尔在人体的药代动力学研究。

Metabolic fate of carteolol hydrochloride, (OPC-1085) VIII, a new beta-adrenergic blocking agent. Pharmacokinetic studies of carteolol in man.

作者信息

Morita S, Iinuma M, Kido M, Sakuragi S, Kohri H, Nishino H

出版信息

Arzneimittelforschung. 1977;27(12):2380-3.

PMID:23800
Abstract

The pharmacokinetics of 5-(3-tert.-butylamino-2-hydroxy)-propoxy-3,4-dihydrocarbostyril hydrochloride (carteolol hydrochloride, OPC-1085) have been investigated in man following single or repetitive oral administration. The plasma half-lives. The plasma half-lives of carteolol at single doses of 10, 15 and 30 mg were 5.4, 5.5 and 5.0 h, respectively. The amounts of carteolol excreted into urine within 24 h at the same dose levels accounted for 64, 70 and 76% of the respective doses. The half-lives obtained by the Sigmaminus method were 5.6, 5.6 and 5.4 h, respectively, being essentially consistent with the aforementioned plasma half-lives of carteolol after administration at 15 mg daily for 7 successive days were determined to be 5.54 h on the 1st day and 6.91 h on the 7th day, displaying the increase in half-life value with the repetitive dosing. While, the predicted value determined using the experimental value on the 1st day agreed with the experimental value on the 7th day. Furthermore, the amounts of carteolol excreted in the urine were not significantly different between the 1st and 7th days. The 7-day repetitive administration with carteolol brought about the steady state of plasma levels. It was concluded from these results that carteolol has little ability to accumulate in man.

摘要

对5-(3-叔丁基氨基-2-羟基)-丙氧基-3,4-二氢卡巴唑盐酸盐(盐酸卡替洛尔,OPC - 1085)在人体单次或重复口服给药后的药代动力学进行了研究。血浆半衰期。单次服用10、15和30毫克卡替洛尔的血浆半衰期分别为5.4、5.5和5.0小时。在相同剂量水平下,24小时内排泄到尿液中的卡替洛尔量分别占各自剂量的64%、70%和76%。通过Sigmaminus方法获得的半衰期分别为5.6、5.6和5.4小时,与上述卡替洛尔给药后的血浆半衰期基本一致。连续7天每天服用15毫克后,第1天的半衰期测定为5.54小时,第7天为6.91小时,显示出重复给药后半衰期值增加。同时,使用第1天的实验值确定的预测值与第7天的实验值一致。此外,第1天和第7天尿液中排泄的卡替洛尔量没有显著差异。卡替洛尔连续7天重复给药使血浆水平达到稳态。从这些结果得出结论,卡替洛尔在人体中几乎没有蓄积能力。

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