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肥胖患者中抗癌药物剂量计算的替代尺寸描述符评估

Evaluation of alternate size descriptors for dose calculation of anticancer drugs in the obese.

作者信息

Sparreboom Alex, Wolff Antonio C, Mathijssen Ron H J, Chatelut Etienne, Rowinsky Eric K, Verweij Jaap, Baker Sharyn D

机构信息

Department of Medical Oncology, Erasmus MC-Daniel den Hoed Cancer Center, Rotterdam, The Netherlands.

出版信息

J Clin Oncol. 2007 Oct 20;25(30):4707-13. doi: 10.1200/JCO.2007.11.2938.

Abstract

PURPOSE

Despite the rising prevalence of obesity, there is paucity of information describing how doses of anticancer drugs should be adjusted in clinical practice. Here, we assessed the pharmacokinetics of eight anticancer drugs in adults and evaluated the potential utility of alternative weight descriptors in dose calculation for the obese.

PATIENTS AND METHODS

A total of 1,206 adult cancer patients were studied, of whom 162 (13.4%) were obese (body mass index > or = 30). Pharmacokinetic parameters were calculated using noncompartmental analysis, and compared between lean (body mass index < or = 25) and obese patients.

RESULTS

The absolute clearance of cisplatin, paclitaxel, and troxacitabine was significantly increased in the obese (P < .023), but this was not observed for carboplatin, docetaxel, irinotecan, or topotecan (P < .17). For doxorubicin, the systemic clearance was statistically significantly reduced in obese women (P = .013), but not in obese men (P = .52). Evaluation of alternate weight descriptors for dose calculation in the obese, including predicted normal weight, lean body mass, (adjusted) ideal body weight, and the mean of ideal and actual body weight, indicated that, for most of the evaluated drugs, weight scalars used to calculate body-surface area should consider actual body weight regardless of size.

CONCLUSION

The results suggest that a number of widely used empiric strategies for dose adjustments in obese patients, including a priori dose reduction or dose capping, should be discouraged.

摘要

目的

尽管肥胖症的患病率不断上升,但关于在临床实践中应如何调整抗癌药物剂量的信息却很少。在此,我们评估了八种抗癌药物在成人中的药代动力学,并评估了替代体重描述符在肥胖患者剂量计算中的潜在效用。

患者与方法

共研究了1206例成年癌症患者,其中162例(13.4%)为肥胖患者(体重指数≥30)。使用非房室分析计算药代动力学参数,并在瘦患者(体重指数≤25)和肥胖患者之间进行比较。

结果

肥胖患者中顺铂、紫杉醇和曲西他滨的绝对清除率显著增加(P<.023),但卡铂、多西他赛、伊立替康或拓扑替康未观察到这种情况(P<.17)。对于阿霉素,肥胖女性的全身清除率在统计学上显著降低(P=.013),但肥胖男性未降低(P=.52)。对肥胖患者剂量计算的替代体重描述符进行评估,包括预测正常体重、瘦体重、(调整后)理想体重以及理想体重与实际体重的平均值,结果表明,对于大多数评估药物,用于计算体表面积的体重标量应考虑实际体重,无论体型如何。

结论

结果表明,应不鼓励使用一些广泛应用于肥胖患者剂量调整的经验性策略,包括预先降低剂量或剂量上限。

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