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5-氟尿嘧啶对结肠癌进行连续5天的区域化疗:药代动力学评估

Continuous 5-day regional chemotherapy by 5-fluorouracil in colon carcinoma: pharmacokinetic evaluation.

作者信息

Boublil J L, Milano G, Khater R, Bourry J, Thyss A, Bruneton J N, Renée N, Philip C, Namer M

出版信息

Br J Cancer. 1985 Jul;52(1):15-20. doi: 10.1038/bjc.1985.142.

Abstract

Eighteen patients with liver metastasis or locoregional recurrence of colon carcinoma received locoregional treatment by continuous 5-day infusions of 5-FU. 5-FU blood levels were measured by HPLC every day of the cycle at 8 am and 5 pm for a total of 87 cycles. Twelve patients were given the drug by an intra-arterial hepatic (i.a.h.) route, 3 by the portal vein (i.p.v.) and 3 by an intra-arterial pelvic (i.a.p.) route. These three routes were compared in respect of their relative pre-systemic drug uptake and the effect of dose escalation. Both the i.a.h. and i.p.v. routes, but not the i.a.p. route, resulted in a significant reduction in AUC 0-105 h compared to the i.v. route at the same dose range. Increasing the dose led to a modification in circulating 5-FU levels proportional to the dose for the i.v. and i.a.p. routes. By contrast, for the i.a.h. and i.p.v. routes, systemic drug delivery was significantly elevated, out of proportion with the dose, indicating a saturable process. For the i.a.h. route, increasing the 5-FU dose from 780 to 1000 mg m-2 day-1 caused a drop in hepatic extraction from 0.93 (0.90-0.95) to 0.44 (0.21-0.66). Liver saturation mechanisms were also evidenced by a mean increase of 2.6 times for the circulating drug level during the second part of the cycle as compared to the first part (P less than 0.001). The evolution of 5-FU AUC 0-105 h as a function of the dose was exponential (r = 0.75, P less than 0.001). Local extraction consecutive to i.a.p. was non-existent, implying that this route of drug administration has no potential advantage over classical i.v. infusion.

摘要

18例结肠癌肝转移或局部区域复发患者接受了为期5天的5-氟尿嘧啶(5-FU)持续输注局部区域治疗。在整个周期的每一天上午8点和下午5点,通过高效液相色谱法(HPLC)测量5-FU血药浓度,共进行了87个周期。12例患者通过肝动脉内(i.a.h.)途径给药,3例通过门静脉(i.p.v.)给药,3例通过盆腔动脉内(i.a.p.)途径给药。比较了这三种途径的相对全身前药物摄取情况以及剂量递增的效果。在相同剂量范围内,与静脉内(i.v.)途径相比,i.a.h.和i.p.v.途径均导致AUC 0-105 h显著降低,但i.a.p.途径未出现这种情况。对于i.v.和i.a.p.途径,增加剂量会导致循环中的5-FU水平按剂量比例变化。相比之下,对于i.a.h.和i.p.v.途径,全身药物递送显著升高,与剂量不成比例,表明存在饱和过程。对于i.a.h.途径,将5-FU剂量从780 mg/m²·天增加到1000 mg/m²·天,导致肝脏摄取率从0.93(0.90-0.95)降至0.44(0.21-0.66)。与周期第一部分相比,周期第二部分循环药物水平平均增加2.6倍,也证明了肝脏饱和机制(P<0.001)。5-FU AUC 0-105 h随剂量的变化呈指数关系(r = 0.75,P<0.001)。i.a.p.途径后不存在局部摄取,这意味着这种给药途径相对于传统静脉输注没有潜在优势。

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