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具有抗肿瘤活性的蛋白激酶抑制剂7-羟基星形孢菌素在小鼠体内的处置情况。

Disposition in mice of 7-hydroxystaurosporine, a protein kinase inhibitor with antitumor activity.

作者信息

Hill D L, Tillery K F, Rose L M, Posey C F

机构信息

Southern Research Institute, Birmingham, AL 35255-5305.

出版信息

Cancer Chemother Pharmacol. 1994;35(1):89-92. doi: 10.1007/BF00686290.

Abstract

UCN-01, a hydroxylated derivative of staurosporine, was selected for study because of its promising antitumor activity. For mice dosed intravenously, subcutaneously, or by oral gavage with this compound, the maximum tolerated doses (MTD) were 20, 10, and > 100 mg/kg, respectively. UCN-01 was stable in mouse and dog plasma, but in human plasma it was converted to a metabolite in a process not inhibited by standard protease and esterase inhibitors. Following an intravenous dose of 10 mg/kg UCN-01, the half-lives for the initial (t1/2 alpha) and terminal (t1/2 beta) exponential phases of elimination were 10 and 85 min, respectively; the area under the plasma concentration-time curve (AUC value) was 117 micrograms min ml-1. In mice dosed by oral gavage with 10 mg/kg, the calculated value for the half-life of the elimination phase was 150 min. The AUC value was 15 micrograms min ml-1, giving a value for bioavailability of 13%. After subcutaneous dosing with 10 mg/kg, the calculated values for half-lives for the distribution and elimination phases were 23 and 130 min, respectively; the AUC value was 113 micrograms min ml-1. Since this value is equivalent to that obtained for intravenous dosing, administration of UCN-01 by the subcutaneous route may be an alternative to intravenous dosing in preclinical and clinical trials.

摘要

UCN - 01是一种星形孢菌素的羟基化衍生物,因其具有良好的抗肿瘤活性而被选作研究对象。对于经静脉注射、皮下注射或灌胃给予该化合物的小鼠,其最大耐受剂量(MTD)分别为20、10和>100 mg/kg。UCN - 01在小鼠和犬血浆中稳定,但在人血浆中会转化为一种代谢产物,此过程不受标准蛋白酶和酯酶抑制剂的抑制。静脉注射10 mg/kg UCN - 01后,消除的初始(t1/2α)和终末(t1/2β)指数相的半衰期分别为10和85分钟;血浆浓度 - 时间曲线下面积(AUC值)为117微克·分钟·毫升-1。对于经灌胃给予10 mg/kg的小鼠,消除相半衰期的计算值为150分钟。AUC值为15微克·分钟·毫升-1,生物利用度为13%。皮下注射10 mg/kg后,分布相和消除相半衰期的计算值分别为23和130分钟;AUC值为113微克·分钟·毫升-1。由于该值与静脉给药所得值相当,在临床前和临床试验中,皮下途径给予UCN - 01可能是静脉给药的一种替代方式。

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