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Number of Regularly Prescribed Drugs and Intrapatient Tacrolimus Trough Levels Variability in Stable Kidney Transplant Recipients

机译:稳定的肾脏移植受者中的常规处方药数量和患者的他克莫司低谷水平变异性

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摘要

High intra-patient variability (IPV) of tacrolimus levels is associated with poor long-term outcome after transplantation. We aimed to evaluate whether the number of regularly prescribed medications is associated with the tacrolimus IPV. We have studied 152 kidney transplant recipients (KTRs) with mean post-transplant time of 6.0 ± 3.1 years. The coefficient of variation (CV) as a measure of IPV was calculated in each individual patient. Data concerning the type and number of currently prescribed medications were collected. The participants were divided into four groups, based on the number of regularly prescribed drugs (≤3, 4–6, 7–9, ≥10 drugs, respectively). There was an increasing trend for median CV, proportional to the increasing number of medications [group 1: 0.11 (interquartile range, 0.08–0.14), group 2: 0.14 (0.01–0.17), group 3: 0.17 (0.14–0.23), group 4: 0.17 (0.15–0.30); value for trend = 0.001]. Stepwise backward multivariate regression analysis revealed that the number of medications [partial correlation coefficient ( ) = 0.503, < 0.001] independently influenced the tacrolimus IPV. Concomitant steroid or diuretics use increased IPV only in Advagraf-treated KTRs, whereas proton-pump inhibitor or statin use increased IPV in the Prograf group but not in the Advagraf group. A large number of concomitant medications significantly increases the tacrolimus IPV in stable KTRs.
机译:他克莫司水平的高患者体内变异性(IPV)与移植后长期预后不良有关。我们旨在评估常规处方药物的数量是否与他克莫司IPV有关。我们研究了152名肾移植受者(KTR),平均移植后时间为6.0±3.1年。计算每位患者的变异系数(CV)作为IPV的量度。收集了有关当前处方药物类型和数量的数据。根据常规处方药的数量将参与者分为四组(分别≤3、4-6、7-9,≥10种药物)。中位CV呈增加趋势,与用药数量成正比[组1:0.11(四分位间距,0.08-0.14),组2:0.14(0.01-0.17),组3:0.17(0.14-0.23),第4组:0.17(0.15–0.30);趋势值= 0.001]。逐步向后的多元回归分析表明,药物的使用[偏相关系数()= 0.503,<0.001]独立地影响了他克莫司的IPV。仅在Advagraf治疗的KTR中,伴随使用类固醇或利尿剂的IPV升高,而在Prograf组中质子泵抑制剂或他汀类药物的IPV升高,而在Advagraf组中则没有。在稳定的KTR中,大量伴随药物显着增加了他克莫司IPV。

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