Veal Gareth J, Errington Julie, Sastry Jairam, Chisholm Julia, Brock Penelope, Morgenstern Daniel, Pritchard-Jones Kathy, Chowdhury Tanzina
Northern Institute for Cancer Research, Paul O'Gorman Building, Medical School, Framlington Place, Newcastle University, Newcastle upon Tyne, NE2 4HH, UK.
School of Medicine, Glasgow University, Glasgow, G12 8QQ, UK.
Cancer Chemother Pharmacol. 2016 Apr;77(4):685-92. doi: 10.1007/s00280-016-2975-0. Epub 2016 Feb 13.
Selection of the most appropriate chemotherapy dosing regimens for neonates treated within the first weeks of life represents a significant clinical dilemma. Due to a lack of information relating to the clinical pharmacology of anticancer drugs in these challenging patients, current dosing guidelines are based on limited scientific rationale. In the current study, we investigate the utilisation of therapeutic drug monitoring approaches in neonates with localised hepatoblastoma, Wilms' tumour and stage 4S neuroblastoma, being treated with widely used anticancer drugs.
Plasma concentrations of cisplatin, vincristine, etoposide and carboplatin were quantified in two neonates being treated within the first 3 weeks of life and in a 32-week preterm infant treated at a gestational age of 40 weeks. Therapeutic drug monitoring was carried out where appropriate, based on the pharmacokinetic data obtained in conjunction with clinical response and toxicity.
Treatment of a child aged 2 weeks with a recommended cisplatin dose reduction for weight to 1.8 mg/kg resulted in achievement of unbound cisplatin plasma concentrations of 0.01-0.08 µg/mL, markedly lower than exposures previously reported in infants and older children. A dose increase to 2.7 mg/kg was implemented, leading to the achievement of levels more in-line with those previously reported. This increased dose level was well tolerated over six courses of treatment, resulting in a good response to cisplatin monotherapy and the patient remains in remission at 3.5 years. In contrast, a 50 % vincristine dose reduction for weight in a 3-week-old neonate resulted in plasma concentrations comparable to levels observed in older children, leading to successful treatment and continued remission at 2 years. In a third patient, etoposide and carboplatin clearance values normalised to body weight were comparable to those reported in older children, resulting in comparatively lower exposures following reduced dosing.
The current report provides unique data on the pharmacokinetics of several widely used anticancer drugs in neonates treated within the first few weeks of life. The provision of these data acts as a useful reference point to support future dosing decisions to be made by clinicians in the treatment of these challenging patients.
为出生后几周内接受治疗的新生儿选择最合适的化疗给药方案是一个重大的临床难题。由于缺乏这些具有挑战性的患者中抗癌药物临床药理学的相关信息,目前的给药指南基于有限的科学依据。在本研究中,我们调查了治疗药物监测方法在接受广泛使用的抗癌药物治疗的局部肝母细胞瘤、肾母细胞瘤和4S期神经母细胞瘤新生儿中的应用。
对出生后3周内接受治疗的两名新生儿以及一名在孕40周时接受治疗的32周早产儿的血浆中顺铂、长春新碱、依托泊苷和卡铂浓度进行定量。根据结合临床反应和毒性获得的药代动力学数据,在适当情况下进行治疗药物监测。
一名2周龄儿童接受推荐的顺铂剂量按体重减至1.8mg/kg治疗,未结合的顺铂血浆浓度达到0.01 - 0.08μg/mL,明显低于先前在婴儿和大龄儿童中报道的暴露水平。将剂量增加至2.7mg/kg后,达到了与先前报道更一致的水平。在六个疗程的治疗中,这种增加的剂量水平耐受性良好,导致对顺铂单药治疗反应良好,患者在3.5岁时仍处于缓解期。相比之下,一名3周龄新生儿的长春新碱剂量按体重减少50%,其血浆浓度与大龄儿童中观察到的水平相当,导致治疗成功并在2岁时持续缓解。在第三名患者中,依托泊苷和卡铂按体重标准化的清除值与大龄儿童中报道的相当,剂量减少后暴露相对较低。
本报告提供了关于几种广泛使用的抗癌药物在出生后几周内接受治疗的新生儿药代动力学的独特数据。这些数据的提供作为一个有用的参考点,以支持临床医生在治疗这些具有挑战性的患者时未来的给药决策。
