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口服替加氟作为5-氟尿嘧啶前体药物的药理学相关性。

Relevance of the pharmacology of oral tegafur to its use as a 5-FU pro-drug.

作者信息

Byfield J E, Hornbeck C L, Frankel S S, Sharp T R, Griffiths J C

出版信息

Cancer Treat Rep. 1985 Jun;69(6):645-52.

PMID:3926308
Abstract

We have studied the pharmacology of iv and oral tegafur (FT) and compared the results with similar studies using continuously infused 5-FU. All patients received daily abdominal irradiation as well as FT. In eight patients receiving 1.0 g/m2 of iv FT, serum FT levels were essentially the same as those in five patients receiving the same dose of oral FT. Oral FT appeared well-absorbed, even with abdominal irradiation. The mean serum FT achieved on a daily basis was a linear function of the oral FT dose between 1.0 and 2.5 g/m2 and was consistently about 1000-fold higher than the resultant 5-FU level. The major FT metabolite, dehydro-FT (DHFT), was persistently present at about ten times the 5-FU level. Because of their long half-lives, both FT and DHFT accumulate during continuous therapy. When the mean serum 5-FU levels with oral FT were compared to those found during continuous 5-FU infusions, we found that oral FT was the equivalent of low-level 5-FU infusion. Oral FT at 1.0 g/m2 was the equivalent of about 11.5 mg/kg/24 hours of 5-FU, increasing to about 17.5 mg/kg of 5-FU for oral FT at 2.5 g/m2. The pharmacologic properties of FT appear to dictate its most useful schedule (continuous oral dosing in multiple doses) and explain why FT alone is not ideal as a 5-FU pro-drug. In addition, insight into the pharmacokinetic limitations of FT also suggests means by which its usage may be improved, including its potential application as a radiosensitizer.

摘要

我们研究了静脉注射和口服替加氟(FT)的药理学,并将结果与使用持续输注5-氟尿嘧啶(5-FU)的类似研究进行了比较。所有患者均接受每日腹部照射以及FT治疗。在8名接受1.0 g/m²静脉注射FT的患者中,血清FT水平与5名接受相同剂量口服FT的患者基本相同。即使接受腹部照射,口服FT的吸收似乎也良好。每日达到的平均血清FT水平是口服FT剂量在1.0至2.5 g/m²之间的线性函数,并且始终比产生的5-FU水平高约1000倍。主要的FT代谢产物,脱氢-FT(DHFT),持续存在的水平约为5-FU水平的10倍。由于它们的半衰期长,FT和DHFT在持续治疗期间都会蓄积。当将口服FT的平均血清5-FU水平与持续输注5-FU期间发现的水平进行比较时,我们发现口服FT相当于低水平的5-FU输注。1.0 g/m²的口服FT相当于约11.5 mg/kg/24小时的5-FU,对于2.5 g/m²的口服FT,增加到约17.5 mg/kg的5-FU。FT的药理特性似乎决定了其最有用的给药方案(多剂量连续口服给药),并解释了为什么单独使用FT作为5-FU前体药物并不理想。此外,对FT药代动力学局限性的深入了解还提示了改善其用法的方法,包括其作为放射增敏剂的潜在应用。

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