大鼠中使用氟尿苷进行离体肺灌注:药代动力学与生存率
Isolated lung perfusion with FUDR in the rat: pharmacokinetics and survival.
作者信息
Port J L, Ng B, Ellis J L, Nawata S, Lenert J T, Burt M E
机构信息
Department of Surgery, Memorial Sloan-Kettering Cancer Center, New York, NY 10021, USA.
出版信息
Ann Thorac Surg. 1996 Sep;62(3):848-52. doi: 10.1016/s0003-4975(96)00508-5.
BACKGROUND
Although surgical resection remains the mainstay of treatment for metastatic pulmonary colorectal cancer, 5-year survival approaches only 30% to 40%. We have developed a model of isolated left lung perfusion (ILP) with FUDR (2'-deoxy-5-fluorouridine) for the treatment of pulmonary colorectal metastases. FUDR ILP toxicity and pharmacokinetics were evaluated and compared with continuous intravenous infusion in the rat.
METHODS
Toxicity was first evaluated in F344 rats (n = 17) after left ILP (20-minute perfusion at 0.5 mL/min) with 21 mg/mL (n = 11), 28 mg/mL (n = 2), 35 mg/mL (n = 2), and 70 mg/mL (n = 2) of FUDR. Animals were followed up and weights recorded for 14 days postoperatively before a right pneumonectomy was performed to evaluate the effect of FUDR perfusion on left lung function. In the second study, 32 rats (n = 8/group) underwent: systemic FUDR (intravenous), or ILP with 7, 14, and 21 mg/mL respectively (ILP 7, ILP 14, and ILP 21 groups). Left lungs and serum were analyzed for FUDR and 5-fluorouracil by high-performance liquid chromatography.
RESULTS
Rats perfused with doses of FUDR greater than 21 mg/mL died perioperatively. All animals perfused at 21 mg/mL survived until day 14, and 8/11 survived a right pneumonectomy. Rats that survived ILP resumed normal weight gain and grooming habits within 1 week. Pharmacokinetic evaluation demonstrated that ILP at 21 mg/mL maximally elevated total lung FUDR and 5-fluorouracil levels (508.5 +/- 96.4 micrograms/g lung) in comparison with the ILP 14, ILP 7, and intravenous groups (299.1 +/- 44.8, 116.0 +/- 21.1, and 7.5 +/- 4.1 micrograms/g lung, respectively) (p < 0.05). Serum FUDR levels were 10.5 +/- 6.8, 1.3 +/- 0.5, 2.31 +/- 1.1, and 1.2 +/- 0.4 microgram/g lung (p = not significant) for intravenous, ILP 7, ILP 14, and ILP 21 groups, respectively.
CONCLUSIONS
Isolated left lung perfusion with FUDR is well tolerated to a maximum dose of 21 mg/mL and results in significantly higher FUDR and 5-fluorouracil lung levels with low serum levels compared with intravenous treatment. These higher pulmonary levels may offer advantages in the treatment of pulmonary colorectal metastases.
背景
尽管手术切除仍是转移性肺结直肠癌治疗的主要手段,但5年生存率仅为30%至40%。我们已开发出一种用氟尿苷(2'-脱氧-5-氟尿苷)进行左肺隔离灌注(ILP)的模型,用于治疗肺结直肠癌转移灶。对氟尿苷ILP的毒性和药代动力学进行了评估,并与大鼠连续静脉输注进行比较。
方法
首先在17只F344大鼠中评估毒性,这些大鼠接受了左肺ILP(以0.5 mL/分钟的速度灌注20分钟),灌注液中氟尿苷的浓度分别为21 mg/mL(n = 11)、28 mg/mL(n = 2)、35 mg/mL(n = 2)和70 mg/mL(n = 2)。对动物进行随访,并在术后14天记录体重,之后进行右肺切除术以评估氟尿苷灌注对左肺功能的影响。在第二项研究中,32只大鼠(每组n = 8)接受:全身氟尿苷(静脉注射),或分别用7、14和21 mg/mL的氟尿苷进行ILP(ILP 7组、ILP 14组和ILP 21组)。通过高效液相色谱法分析左肺和血清中的氟尿苷和5-氟尿嘧啶。
结果
灌注氟尿苷剂量大于21 mg/mL的大鼠在围手术期死亡。所有以21 mg/mL灌注的动物均存活至第14天,11只中有8只存活至右肺切除术后。接受ILP后存活的大鼠在1周内恢复了正常的体重增加和梳理习惯。药代动力学评估表明,与ILP 14组、ILP 7组和静脉注射组相比,21 mg/mL的ILP使肺内氟尿苷和5-氟尿嘧啶总水平最高升高(508.5±96.4微克/克肺组织)(分别为299.1±44.8、116.0±21.1和7.5±4.1微克/克肺组织)(p < 0.05)。静脉注射组、ILP 7组、ILP 14组和ILP 21组的血清氟尿苷水平分别为10.5±6.8、1.3±0.5、2.31±1.1和1.2±0.4微克/克肺组织(p无显著性差异)。
结论
氟尿苷左肺隔离灌注最大剂量为21 mg/mL时耐受性良好,与静脉治疗相比,可使肺内氟尿苷和5-氟尿嘧啶水平显著升高,血清水平较低。这些较高的肺内水平可能在肺结直肠癌转移灶的治疗中具有优势。
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