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他克莫司患者内变异对肾移植临床结局影响的综合评价

A comprehensive review of the impact of tacrolimus intrapatient variability on clinical outcomes in kidney transplantation.

机构信息

Department of Surgery, Medical University of South Carolina, Charleston, SC, USA.

Department of Nursing Operating, Medical University of South Carolina, Charleston, SC, USA.

出版信息

Am J Transplant. 2020 Aug;20(8):1969-1983. doi: 10.1111/ajt.16002. Epub 2020 Jun 17.

Abstract

Tacrolimus (Tac) is widely used to prevent rejection and graft loss in solid organ transplantation. A limiting characteristic of Tac is the high intra and interpatient variability associated with its use. Routine therapeutic drug monitoring (TDM) is necessary to facilitate Tac management and to avoid undesirable clinical outcomes. However, whole blood trough concentrations commonly utilized in TDM are not strong predictors of the detrimental clinical outcomes of interest. Recently, researchers have focused on Tac intrapatient variability (Tac IPV) as a novel marker to better assess patient risk. Higher Tac IPV has been associated with a number of mechanisms leading to shortened graft survival. Medication nonadherence (MNA) is considered to be the primary determinant of high Tac IPV and perhaps the most modifiable risk factor. An understanding of the methodology behind Tac IPV is imperative to its recognition as an important prognostic measure and integration into clinical practice. Therapeutic interventions targeting MNA and reducing Tac IPV are crucial to improving long-term graft survival.

摘要

他克莫司(Tac)广泛用于预防实体器官移植中的排斥反应和移植物丢失。Tac 的一个限制特征是与使用相关的高个体内和个体间变异性。常规治疗药物监测(TDM)对于促进 Tac 的管理和避免不良临床结局是必要的。然而,在 TDM 中常用的全血谷浓度并不是对感兴趣的不良临床结局的强有力预测指标。最近,研究人员将 Tac 个体内变异性(Tac IPV)作为一种新的标志物来更好地评估患者的风险。较高的 Tac IPV 与导致移植物存活时间缩短的多种机制有关。药物不依从(MNA)被认为是 Tac IPV 升高的主要决定因素,也是最可改变的危险因素。了解 Tac IPV 背后的方法学对于将其识别为重要的预后指标并纳入临床实践至关重要。针对 MNA 的治疗干预措施和降低 Tac IPV 对于提高长期移植物存活率至关重要。

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