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高通量血液透析增强环磷酰胺清除率:一例管型肾病患者的单剂量药代动力学研究

Enhanced elimination of cyclophosphamide by high cut-off haemodialysis: single-dose pharmacokinetics in a patient with cast nephropathy.

作者信息

Eden Gabriele, Kühn-Velten W Nikolaus, Hafer Carsten, Kielstein Jan T

机构信息

Medical Clinic V Nephrology | Rheumatology | Blood Purification, Academic Teaching Hospital Braunschweig, Braunschweig, Germany.

Medizinisches Labor Bremen, Bremen, Germany.

出版信息

BMJ Case Rep. 2018 Jan 4;2018:bcr-2017-221735. doi: 10.1136/bcr-2017-221735.

Abstract

High cut-off (HCO) haemodialysis removes free light chains in patients with multiple myeloma. This is possible as HCO dialysers allow clearance of molecules up to a molecular weight of 65 kDa. In contrast, high-flux dialysers, which are used in routine haemodialysis, only remove molecules up to a molecular weight of 20 kDa. Even though patients with advanced myeloma frequently need dialysis and alkylating agents, drug dosing recommendations in this patient population are scarce at best or absent as for cyclophosphamide dosing in patients with myeloma undergoing HCO dialysis. Therefore, we aimed to determine pharmacokinetics of cyclophosphamide in a 52-year-old man (height 172 cm, weight 80 kg) with cast nephropathy. Intermittent 4-hour haemodialysis was started ~6 hours after the end of a 70 min cyclophosphamide infusion containing 1700 mg of this drug. Blood/dialysate flow rates were 300/500 mL/hour, respectively. Peak concentration of cyclophosphamide was 24.7 mg/L. Using HCO dialysis, plasma concentration of cyclophosphamide decreased from 10.8 mg/L to 3.7 mg/L during the treatment. The calculated whole blood dialyser clearance was 166 mL/min. HCO dialysis led to a marked decrease of cyclophosphamide resulting in a a 50% reduction in half-life as compared with the half-life before dialysis. This removal has to be accounted for in dosing cyclophosphamide.

摘要

高通量(HCO)血液透析可清除多发性骨髓瘤患者的游离轻链。这是可行的,因为HCO透析器能够清除分子量高达65 kDa的分子。相比之下,常规血液透析中使用的高通量透析器仅能清除分子量达20 kDa的分子。尽管晚期骨髓瘤患者经常需要透析和使用烷化剂,但针对这一患者群体的药物剂量推荐充其量也很稀少,对于接受HCO透析的骨髓瘤患者使用环磷酰胺的剂量推荐甚至缺失。因此,我们旨在确定一名52岁男性(身高172 cm,体重80 kg)患有管型肾病时环磷酰胺的药代动力学。在输注含1700 mg环磷酰胺的溶液70分钟结束后约6小时开始间歇性4小时血液透析。血液/透析液流速分别为300/500 mL/小时。环磷酰胺的峰值浓度为24.7 mg/L。使用HCO透析时,治疗期间环磷酰胺的血浆浓度从10.8 mg/L降至3.7 mg/L。计算得出的全血透析器清除率为166 mL/分钟。HCO透析导致环磷酰胺显著减少,与透析前的半衰期相比,半衰期缩短了50%。在给予环磷酰胺时必须考虑这种清除情况。

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Saving two lives with one dialysis treatment.一次透析治疗挽救两条生命。
Clin Nephrol. 2015 Aug;84(2):104-7. doi: 10.5414/CN108441.
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Clinical pharmacokinetics of cyclophosphamide.环磷酰胺的临床药代动力学
Clin Pharmacokinet. 1991 Mar;20(3):194-208. doi: 10.2165/00003088-199120030-00002.

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