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饮食诱导的肥胖改变了小鼠血液和组织中长春新碱的药代动力学。

Diet-induced obesity alters vincristine pharmacokinetics in blood and tissues of mice.

机构信息

Division of Endocrinology, Diabetes & Metabolism, Childrens Hospital Los Angeles, 4650 Sunset Boulevard, Los Angeles, CA 90027, USA.

出版信息

Pharmacol Res. 2010 May;61(5):385-90. doi: 10.1016/j.phrs.2010.01.007. Epub 2010 Jan 18.

Abstract

Obesity is associated with poorer outcome from many cancers, including leukemia. One possible contributor to this could be suboptimal chemotherapy dosing in obese patients. We have previously found that vincristine (VCR) is less effective in obese compared to non-obese mice with leukemia, despite weight-based dosing. In the present study, we administered (3)H-VCR to obese and control mice to determine whether obesity would cause suboptimal VCR exposure. Blood VCR concentrations were fitted with a three-compartment model using pharmacokinetic analysis (two-stage PK) in three subsets of VCR concentrations vs. time method. Tissue and blood VCR concentrations were also analyzed using non-compartmental modeling. Blood VCR concentrations showed a triexponential decay and tended to be slightly higher in the obese mice at all time-points. However, the t(1/2,beta) and t(1/2,gamma) were shorter in the obese mice (9.7 min vs. 44.5 min and 60.3h vs. 85.6h, respectively), resulting in a lower AUC(0-infinity) (13,099 ng/m Lh vs. 15,384 ng/mL h). Had the dose of VCR been "capped", as is done in clinical practice, the AUC(0-infinity) would have been 36% lower in the obese mice than the controls. Tissue disposition of VCR revealed a biexponential decay from spleen, liver, and adipose. Interestingly, VCR slowly accumulated in the bone marrow of control mice, but had a slow decay from the marrow in the obese mice. Thus, obesity alters VCR PK, causing a lower overall exposure in circulation and bone marrow. Given the high prevalence of obesity, additional PK studies should be performed in obese subjects to optimize chemotherapy dosing regimens.

摘要

肥胖与许多癌症(包括白血病)的预后较差有关。肥胖患者可能存在化疗药物剂量不理想的情况。我们之前发现,肥胖荷白血病小鼠对长春新碱(VCR)的敏感性低于非肥胖小鼠,尽管按体重给药。在本研究中,我们给肥胖和对照小鼠给予(3)H-VCR,以确定肥胖是否会导致 VCR 暴露不足。采用两阶段药代动力学分析(two-stage PK)对三个 VCR 浓度与时间方法子集进行分析,拟合血药浓度的三室模型。采用非房室模型分析组织和血药 VCR 浓度。血药 VCR 浓度呈三指数衰减,在所有时间点肥胖小鼠的浓度均略高。然而,肥胖小鼠的 t(1/2,beta)和 t(1/2,gamma)更短(分别为 9.7 分钟对 44.5 分钟和 60.3 小时对 85.6 小时),导致 AUC(0-infinity)降低(13099ng/mLh 对 15384ng/mL h)。如果按临床实践中“封顶”VCR 剂量,肥胖小鼠的 AUC(0-infinity)将比对照组低 36%。VCR 的组织分布呈双指数衰减,从脾、肝和脂肪中排泄。有趣的是,VCR 缓慢积聚在对照小鼠的骨髓中,但在肥胖小鼠的骨髓中迅速衰减。因此,肥胖改变了 VCR 的药代动力学,导致循环和骨髓中的总体暴露量降低。鉴于肥胖的高患病率,应在肥胖受试者中进行额外的 PK 研究,以优化化疗剂量方案。

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