首页> 外文期刊>Biological & pharmaceutical bulletin >Evidence of different pharmacokinetics including relationship among AUC, peak, and trough levels between cyclosporine and tacrolimus in renal transplant recipients using new pharmacokinetic parameter - Why cyclosporine is monitored by C-2 level and t
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Evidence of different pharmacokinetics including relationship among AUC, peak, and trough levels between cyclosporine and tacrolimus in renal transplant recipients using new pharmacokinetic parameter - Why cyclosporine is monitored by C-2 level and t

机译:使用新的药代动力学参数,肾移植受者中不同药代动力学的证据,包括AUC,环孢素和他克莫司之间的峰值和谷值之间的关系-为什么通过C-2水平和t监测环孢素

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摘要

The clinical efficacy of calcineurin inhibitors administered to renal transplant patients is considered to be a strong function of the area under the concentration time curve (AUC). Interestingly, monitoring timings of blood concentrations for two similar calcineurin inhibitors, cyclosporine (CYA; Neoral((R))) and tacrolimus (TAC; Prograf((R))) are different. Namely, CYA blood concentration is usually monitored at 2 h after administration (C-2) substituted for peak concentration (C-p) and TAC at trough concentration (C-1). In the literature, data describing such characteristics of CYA and TAC have been presented in the past. However, each of these patient groups had different backgrounds. We have attempted to examine the behavior of blood concentration curves simultaneously for both CYA and TAC by establishing controlled groups of renal transplant patients with similar clinical backgrounds. Furthermore, we have analyzed the correlation with C-P and C-1 versus AUC implementing area under the trough level (AUTL), or area above the trough level (AATL) as new pharmacokinetic parameters, such that C, for CYA and C-1 for TAC have been verified using controlled clinical data. We have also found distinct differences in the pharmacokinetics between CYA and TAC with the relationships between AUC, C-p, and C-1.
机译:给予肾移植患者的钙调神经磷酸酶抑制剂的临床功效被认为是浓度时间曲线(AUC)下面积的强大功能。有趣的是,两种相似的钙调神经磷酸酶抑制剂环孢素(CYA; Neoral(R))和他克莫司(TAC; Prograf(R))的血药浓度监测时机不同。即,通常在给药后2小时(C-2)代替峰浓度(C-p)和谷浓度(C-1)的TAC监测CYA血液浓度。在文献中,过去已经提供了描述CYA和TAC此类特征的数据。但是,每个这些患者组都有不同的背景。我们试图通过建立具有相似临床背景的肾移植患者的对照组来同时检查CYA和TAC的血药浓度曲线的行为。此外,我们已经分析了与CP和C-1相对于谷值以下(AUTL)或AUC谷以上的面积(AATL)的实施面积的相关性,将其作为新的药代动力学参数,例如CYA和C-1用于TAC已使用可控的临床数据进行了验证。我们还发现CYA和TAC之间的药代动力学存在明显差异,并且AUC,C-p和C-1之间的关系也不同。

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