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心脏移植患者从标准他克莫司转换为缓释他克莫司需要增加剂量。

Conversion of heart transplant patients from standard to sustained-release tacrolimus requires a dosage increase.

作者信息

Marzoa-Rivas R, Paniagua-Martín M J, Barge-Caballero E, Pedrosa del Moral V, Barge-Caballero G, Grille-Cancela Z, Naya-Leira C, Fariñas-Garrido P, Blanco-Canosa P, Mosquera V, Castro-Beiras A, Crespo-Leiro M G

机构信息

Advanced Heart Failure and Heart Transplant Unit, Hospital Universitario A Coruña, A Coruña, Spain.

出版信息

Transplant Proc. 2010 Oct;42(8):2994-6. doi: 10.1016/j.transproceed.2010.08.020.

DOI:10.1016/j.transproceed.2010.08.020
PMID:20970591
Abstract

INTRODUCTION

It has been suggested that for adequate maintenance of tacrolimus levels, the total daily dosage should be increased when switching from the conventional twice-daily regimen tacrolimus (CT) to once-daily sustained-release tacrolimus (SR-T).

OBJECTIVE

To evaluate the safety and efficacy of a 25% increase in daily dosage when switching heart transplant (HT) patients from CT to SR-T.

METHODS

We switched 75 HT patients including 72% males and an overall mean age of 55.6 years from CT to SR-T using a 25% increase in daily dosage. We screened for adverse events by measurements of lipids, creatinine, glycemia, and tacrolimus in blood samples taken at 1, 3, 7, and 12 weeks after the conversion, as well as by repeated echocardiography and routine clinical examinations.

RESULTS

Just two patients (2.7%) were returned to CT because of failure of SR-T to attain therapeutic levels. In the remainder of subjects, tacrolimus levels remained stable, with trough values of 8.7±3.2, 8.7±2.9, 8.3±2.6, and 7.5±2.0 mg/dL, respectively. Twenty-three patients (31%) required no dosage change in the first 3 months, but 44 (33%) required one or two changes. No departure from therapeutic levels was associated with rejection; there was no case of severe intercurrent infection. We did not observe significant changes in glycemia, creatinine, lipid profile, or blood pressure.

CONCLUSIONS

Administration of SR-T at a dosage 25% higher than the daily dosage of CT was safe. It ensured adequate tacrolimus levels in one-third of patients. Nevertheless, strict analytical surveillance is necessary during the initial months to allow dosage adjustments and to detect the minority of patients for whom SR-T does not achieve therapeutic tacrolimus levels.

摘要

引言

有人提出,为了充分维持他克莫司的血药浓度,从传统的他克莫司每日两次给药方案(CT)转换为他克莫司每日一次缓释制剂(SR-T)时,应增加每日总剂量。

目的

评估心脏移植(HT)患者从CT转换为SR-T时,每日剂量增加25%的安全性和有效性。

方法

我们将75例HT患者(其中72%为男性,总体平均年龄55.6岁)从CT转换为SR-T,每日剂量增加25%。在转换后1、3、7和12周采集血样,通过检测血脂、肌酐、血糖和他克莫司来筛查不良事件,同时进行重复超声心动图检查和常规临床检查。

结果

仅2例患者(2.7%)因SR-T未能达到治疗浓度而恢复使用CT。在其余患者中,他克莫司血药浓度保持稳定,谷值分别为8.7±3.2、8.7±2.9、8.3±2.6和7.5±2.0mg/dL。23例患者(31%)在最初3个月无需调整剂量,但44例患者(33%)需要进行一到两次剂量调整。未出现与排斥反应相关的治疗浓度偏离情况;未发生严重并发感染病例。我们未观察到血糖、肌酐、血脂谱或血压有显著变化。

结论

以高于CT每日剂量25%的剂量给予SR-T是安全的。它确保了三分之一患者的他克莫司血药浓度充足。然而,在最初几个月需要进行严格的分析监测,以便调整剂量并发现少数SR-T未能达到治疗性他克莫司血药浓度的患者。

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