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首页> 外文期刊>Therapeutic Drug Monitoring >A limited sampling model for estimation of total and unbound mycophenolic acid (MPA) area under the curve (AUC) in hematopoietic cell transplantation (HCT).
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A limited sampling model for estimation of total and unbound mycophenolic acid (MPA) area under the curve (AUC) in hematopoietic cell transplantation (HCT).

机译:一种有限的采样模型,用于估计造血细胞移植(HCT)中曲线下的总和未结合的麦考酚酸(MPA)面积(AUC)。

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OBJECTIVES: Renal transplant patients with suboptimal mycophenolic acid (MPA) areas under the curves (AUCs) are at greater risk of acute rejection. In hematopoietic cell transplantation, a low MPA AUC is also associated with a higher incidence of acute graft versus host disease. Therefore, a limited sampling model was developed and validated to simultaneously estimate total and unbound MPA AUC0-12 in hematopoietic cell transplantation patients. METHODS: Intensive pharmacokinetic sampling was performed at steady state between days 3 to 7 posttransplant in 73 adult subjects while receiving prophylactic mycophenolate mofetil 1 g per 12 hours orally or intravenously plus cyclosporine. Total and unbound MPA plasma concentrations were measured, and total and unbound AUC0-12 was determined using noncompartmental analysis. Regression analysis was then performed to build IV and PO, total and unbound AUC0-12 models from the first 34 subjects. The predictive performance of these models was tested in the next 39 subjects. RESULTS: Trough concentrations poorly estimate observed total and unbound AUC0-12 (r<0.48). A model with 3 concentrations (2-, 4-, and 6-hour post start of infusion) best estimated observed total and unbound AUC0-12 after IV dosing (r>0.99). Oral total and unbound AUC0-12 was more difficult to estimate and required at least 4 concentrations (0-, 1-, 2-, and 6-hour post dose) in the model (r>0.85). The predictive performance of the final models was good. Eighty-three percent of IV and 70% of PO AUC0-12 predictions fell within +/-20% of the observed values without significant bias. CONCLUSION: Trough MPA concentrations do not accurately describe MPA AUC0-12. Three intravenous (2-, 4-, 6-hour post start of infusion) or 4 oral (0-, 1-, 2-, and 6-hour post dose) MPA plasma concentrations measured over a 12-hour dosing interval will estimate the total and unbound AUC0-12 nearly as well as intensive pharmacokinetic sampling with good precision and low bias. This approach simplifies AUC0-12 targeting of MPApost hematopoietic cell transplantation.
机译:目的:在曲线(AUC)下具有次优霉酚酸(MPA)面积的肾移植患者,发生急性排斥反应的风险更大。在造血细胞移植中,低MPA AUC还与急性移植相比宿主疾病发生率更高有关。因此,开发并验证了有限的采样模型,以同时估算造血细胞移植患者的总和未结合的MPA AUC0-12。方法:在73名成年受试者中,于移植后第3天至第7天之间,在稳态下进行了密集的药代动力学采样,同时每12小时口服或静脉内加环孢素1 g预防性霉酚酸酯1 g。测量总和未结合的MPA血浆浓度,并使用非房室分析确定总和未结合的AUC0-12。然后进行回归分析以建立前34名受试者的IV和PO,总和未结合的AUC0-12模型。在接下来的39个受试者中测试了这些模型的预测性能。结果:低谷浓度很难估计观察到的总和未结合的AUC0-12(r <0.48)。在静脉内给药后,具有3种浓度(开始输注后2、4和6小时)的模型可以最佳地估计观察到的总量和未结合的AUC0-12(r> 0.99)。口服的总和未结合的AUC0-12更难以估计,并且在模型中至少需要4种浓度(给药后0、1、2、6小时)(r> 0.85)。最终模型的预测性能良好。 IV的百分之八十三和PO AUC0-12预测的百分之七十落在观测值的+/- 20%之内,而没有明显的偏差。结论:低谷MPA浓度不能准确描述MPA AUC0-12。在12个小时的给药间隔内测得的三个静脉注射(开始输注后2、4、6小时)或4口服(给药后0、1、2、6小时)MPA血浆浓度总和未结合的AUC0-12几乎以及精确度和低偏倚的密集药代动力学采样。该方法简化了MPApost造血细胞移植的AUC0-12靶向。

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