癌症患者口服5'-脱氧-5-氟尿苷的药代动力学和生物利用度
Pharmacokinetics and bioavailability of oral 5'-deoxy-5-fluorouridine in cancer patients.
作者信息
Van Der Heyden S A, Highley M S, De Bruijn E A, Tjaden U R, Reeuwijk H J, Van Slooten H, Van Oosterom A T, Maes R A
机构信息
Laboratory for Experimental Oncology, University of Leuven, B-3000 Leuven, Belgium.
出版信息
Br J Clin Pharmacol. 1999 Apr;47(4):351-6. doi: 10.1046/j.1365-2125.1999.00899.x.
AIMS
Oral administration of 5-fluorouracil (FUra), an important cytotoxic agent, is limited by a wide variation in bioavailability. 5'-deoxy-5-fluorouridine (dFUrd), a masked form of FUra, has shown promise clinically when given intravenously or orally as a solution or tablet. This study investigates the efficacy of an oral capsule formulation of dFUrd in generating continuous systemic levels of this compound in cancer patients.
METHODS
Six patients with advanced intestinal or ovarian malignancies were given three cycles of dFUrd, days 1-5, at intervals of 4 weeks. The doses of dFUrd were 600 mg m-2 three times daily, 800 mg m-2 three times daily, and 1000 mg m-2 three times daily, on cycles one, two and three, respectively (total dose 36 g m-2 ). The initial dose in each cycle was given as a slow intravenous injection over 10 min, and the remainder orally. Plasma and urine levels of dFUrd and two of its metabolites, FUra and 5,6-dihydro-5-fluorouracil (FUraH2 ), were monitored in six patients at each dose level.
RESULTS
All six patients completed the study, receiving three different doses over a 3 month period, following which one had achieved a partial response, one had stable disease, and four had developed progressive disease. Side-effects were negligible, and only two instances of transient diarrhoea WHO grade 1 were seen. Total body clearance (CLtot) of intravenous dFUrd decreased with increasing dose; 2.7, 2.0 and 1.3 l min-1 m-2, following doses of 600, 800 and 1000 mg m-2, respectively. The mean elimination half-life of intravenous dFUrd increased with the dose from 15 to 22 min. Oral dFUrd was rapidly absorbed with a lag time of less than 20 min. The mean elimination half-life (t1/2, z ) of oral dFUrd was 32-45 min in the dose range 600-1000 mg m-2. The AUC of FUra and FUraH2 increased overproportionally with increasing intravenous doses of dFUrd. The mean systemic bioavailability of oral dFUrd was 34-47%.
CONCLUSIONS
dFUrd, which selectively releases the antimetabolite FUra in tumour cells, can be given orally at doses of 600-1000 mg m-2 three times daily for 5 days. The systemic levels achieved are equivalent to those seen following continuous infusions of dFUrd or FUra. Toxicity is tolerable, and further clinical investigation of oral dFUrd is warranted.
目的
5-氟尿嘧啶(FUra)是一种重要的细胞毒性药物,口服给药时生物利用度差异很大,限制了其应用。5'-脱氧-5-氟尿苷(dFUrd)是FUra的一种掩蔽形式,静脉注射或口服溶液或片剂时在临床上已显示出前景。本研究调查了dFUrd口服胶囊制剂在癌症患者中产生该化合物持续全身水平的疗效。
方法
6例晚期肠道或卵巢恶性肿瘤患者,在第1 - 5天给予3个周期的dFUrd,间隔4周。dFUrd的剂量在第1、2和3周期分别为600mg/m²每日3次、800mg/m²每日3次和1000mg/m²每日3次(总剂量36g/m²)。每个周期的初始剂量通过10分钟缓慢静脉注射给药,其余口服。在每个剂量水平对6例患者监测dFUrd及其两种代谢产物FUra和5,6 - 二氢-5-氟尿嘧啶(FUraH2)的血浆和尿液水平。
结果
所有6例患者完成了研究,在3个月内接受了3种不同剂量的治疗,之后1例患者达到部分缓解,1例病情稳定,4例病情进展。副作用可忽略不计,仅观察到2例WHO 1级短暂腹泻。静脉注射dFUrd的全身清除率(CLtot)随剂量增加而降低;分别给予600、800和1000mg/m²剂量后,CLtot为2.7、2.0和1.3l/min/m²。静脉注射dFUrd的平均消除半衰期随剂量从15分钟增加到22分钟。口服dFUrd吸收迅速,滞后时间小于20分钟。在600 - 1000mg/m²剂量范围内,口服dFUrd的平均消除半衰期(t1/2,z)为32 - 45分钟。FUra和FUraH2的曲线下面积(AUC)随静脉注射dFUrd剂量增加而成比例增加。口服dFUrd的平均全身生物利用度为34 - 47%。
结论
dFUrd可在肿瘤细胞中选择性释放抗代谢物FUra,可每日3次口服,剂量为600 - 1000mg/m²,共5天。达到的全身水平与持续输注dFUrd或FUra后的水平相当。毒性可耐受,有必要对口服dFUrd进行进一步的临床研究。
Zotero 插件