Blaney S M, Cole D E, Balis F M, Godwin K, Poplack D G
Walter Reed Army Medical Center, Washington, DC 20307.
Cancer Res. 1993 Feb 15;53(4):725-7.
Topotecan, a water soluble semisynthetic analogue of camptothecin, is a topoisomerase I inhibitor that has recently entered phase II clinical trials. Topotecan has shown significant preclinical activity in refractory murine tumors and in human tumor xenograft models. In addition, objective antineoplastic activity has been observed in recent adult phase I clinical trials. Topotecan is unstable in solution and is rapidly and spontaneously converted to a less active open ring form which predominates at physiological pH. This study was undertaken to better define the pharmacokinetic behavior of this highly unstable compound in both plasma and cerebrospinal fluid (CSF) and to measure the degree of CSF penetration of this novel antineoplastic agent. Three nonhuman primates with indwelling Ommaya reservoirs received 10 mg/m2 i.v. topotecan administered as a 10-min infusion. Frequent plasma and CSF samples were obtained and immediately extracted and assayed with a reverse phase high performance liquid chromatography assay to quantitate the concentration of topotecan (lactone). Samples were then acidified and reinjected to quantitate total drug (lactone ring plus open ring). Peak plasma concentrations of topotecan ranged from 0.27 to 0.45 microM. Plasma disappearance of the lactone ring was biexponential with a distribution half-life (t1/2 alpha) of 22 +/- 5 min and an elimination half-life (t1/2 beta) of 1.3 +/- 0.1 h. Total body clearance of topotecan was 72.1 +/- 15.8 liters/h/m2. The volume of distribution at steady state was 88.6 +/- 33.2 liters/m2. Peak CSF concentrations of topotecan occurred at 30 min following drug administration and ranged from 0.044 to 0.074 microM. CSF disappearance paralleled that in plasma. The mean ratio of the area under the CSF concentration-time curve to that in plasma was 0.32 (range, 0.29 to 0.37). The mean CSF penetration of topotecan exceeds 30%, which is significantly greater than the penetration of most structurally similar chemotherapeutic agents. The impact of chemotherapy on the survival of patients with primary or metastatic central nervous system malignancies is very limited. Therefore, this novel antineoplastic agent is an excellent candidate for further study in patients with high risk or refractory central nervous system tumors.
拓扑替康是喜树碱的一种水溶性半合成类似物,是一种拓扑异构酶I抑制剂,最近已进入II期临床试验。拓扑替康在难治性小鼠肿瘤和人类肿瘤异种移植模型中已显示出显著的临床前活性。此外,在最近的成人I期临床试验中也观察到了客观的抗肿瘤活性。拓扑替康在溶液中不稳定,会迅速自发地转化为活性较低的开环形式,这种形式在生理pH值下占主导。本研究旨在更好地确定这种高度不稳定化合物在血浆和脑脊液(CSF)中的药代动力学行为,并测量这种新型抗肿瘤药物的脑脊液渗透程度。三只植入奥马亚贮器的非人灵长类动物接受了10mg/m²的静脉注射拓扑替康,输注时间为10分钟。频繁采集血浆和脑脊液样本,并立即提取,用反相高效液相色谱法测定以定量拓扑替康(内酯)的浓度。然后将样本酸化并重新进样以定量总药物(内酯环加开环)。拓扑替康的血浆峰值浓度范围为0.27至0.45微摩尔/升。内酯环的血浆消除呈双指数形式,分布半衰期(t1/2α)为22±5分钟,消除半衰期(t1/2β)为1.3±0.1小时。拓扑替康的全身清除率为72.1±15.8升/小时/平方米。稳态分布容积为88.6±33.2升/平方米。拓扑替康的脑脊液峰值浓度在给药后30分钟出现,范围为0.044至0.074微摩尔/升。脑脊液的消除与血浆相似。脑脊液浓度-时间曲线下面积与血浆中该曲线下面积的平均比值为0.32(范围为0.29至0.37)。拓扑替康的平均脑脊液渗透率超过30%,显著高于大多数结构相似的化疗药物的渗透率。化疗对原发性或转移性中枢神经系统恶性肿瘤患者生存的影响非常有限。因此,这种新型抗肿瘤药物是高危或难治性中枢神经系统肿瘤患者进一步研究的极佳候选药物。
