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Pharmacokinetic evaluation of MFF in combinations with tacrolimus and cyclosporine. Findings of C0 and AUC

机译:躯干血管孢菌组合中的MFF药代动力学评价。 C0和AUC的结果

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We hypothesized that area under the concentration time curve (AUC (0-12) ) is more accurate pharmacokinetic predictor vs trough level of mycophenolic acid (C 0 ). Study was performed at the University Hospital of Limoges (France) and included 238 renal recipients aged 22 to 82 years. Risk of nephropathy was evaluated by analyzing data of protocol biopsies according to the Banff 97 classification. Assessment of immunosuppressants’ exposures was based on the calculation of the mean of AUC (0-12) . The AUC (0-12) was estimated using a Bayesian estimator and a 3-point limited sampling strategy. Cyclosporine and tacrolimus analyses were performed using liquid chromatography–mass spectrometry method. The measurement of total mycophenolic acid was performed using a validated high-performance liquid chromatography method with ultraviolet detection. IBM SPSS 20.0 was used for statistical analysis. The most accurate dosing of mycophenolate mofetil ( MMF ) was observed in patients receiving MMF with tacrolimus , 70.6% of patients’ AUC (0-12) exposures were within the therapeutic range. The highest rates of low dosing were observed in patients receiving MMF with cyclosporine , 30.9% of patients had AUC (0-12) exposures below the therapeutic range. The assessment of AUC (0-12) revealed 38% of chronic nephropathy cases, while C 0 enables to identify only 20% of chronic nephropathy cases. Probability test results showed that more likely AUC (0-12) and C 0 will be maintained within the therapeutic width if patients receive MMF with tacrolimus vs MMF with cyclosporine : 0.6320 vs 0.6410 for AUC (0-12) determination and 0.8415 vs 0.4827 for C 0 determination. Combination of MMF with tacrolimus is dosed more precisely vs dosing of MMF with cyclosporine . 72 (70.6%) patients AUC (0-12) and 79 (77.5%) patients C 0 out of 102 patients were within the therapeutic range. The AUC (0-12) monitoring of mycophenolic acid in patients receiving MMF with tacrolimus or in patients receiving MMF with cyclosporine enabled to identify more overdosing and possible risky cases. Study results show that standard MMF dosing without monitoring and with mycophenolic acid level within the therapeutic width is possible and demonstrates less risky cases in patients receiving MMF with tacrolimus , while patients receiving MMF with cyclosporine should be intensively monitored to achieve the highest safety. However, AUC (0-12) monitoring is advised showing better compliance vs C 0 monitoring.
机译:我们假设浓度时间曲线(AUC(0-12))下的区域是更准确的药代动力学预测因子与霉酚酸的槽水平(C 0)。学习在大学(法国)的大学(法国)进行,包括238名肾脏受体22至82岁。根据班夫97分类,通过分析协议活检数据来评估肾病风险。免疫抑制剂的评估是基于计算AUC(0-12)的平均值的计算。使用贝叶斯估计器和3分有限的采样策略估算AUC(0-12)。使用液相色谱 - 质谱法进行环孢菌素和巨杆菌分析。使用具有紫外检测的验证的高效液相色谱法进行总霉酚酸的测量。 IBM SPSS 20.0用于统计分析。在接受MMF的患者中,观察到MMF的患者中最精确的霉菌剂量给药,70.6%的患者的AUC(0-12)曝光在治疗范围内。在接受Cycosporine接受MMF的患者中观察到低给药率的最高速率,30.9%的患者在治疗范围以下的曝光(0-12)曝光。 AUC(0-12)的评估显示38%的慢性肾病病例,而C 0能够识别慢性肾病病例的20%。概率试验结果表明,如果患者接受具有环孢菌素的Tacrolimus与MMF的MMF接受MMF的治疗宽度,则更有可能在治疗宽度内维持:0.6320 Vs 0.6410,用于AUC(0-12)测定,0.8415 Vs 0.4827 C 0确定。 MMF与Tacrolimus的组合更精确地给予MMF与环孢菌素的混合物。 72(70.6%)患者AUC(0-12)和79名(77.5%)患者102名患者的患者在治疗范围内。 AUC(0-12)监测MMF与巨蟹蛋白的MMF接受MMF的患者监测MMF,使MMF接受环孢菌素的患者,以鉴定更多的过度过量和可能的风险性情况。研究结果表明,在治疗宽度内没有监测和霉菌酸水平的标准MMF给药是可能的,并且在接受躯干血症的患者中表现出较小的风险案例,而应密集接受具有环孢菌素的MMF的患者以实现最高安全性。但是,建议AUC(0-12)监测显示更好的合规性与C 0监控。

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