Tacrolimus Dose Requirement in De Novo Adult Kidney Transplant Patients Treated With Adoport® Can Be Anticipated.

IF 2.7 3区 医学 Q1 SURGERY
Transplant International Pub Date : 2024-10-14 eCollection Date: 2024-01-01 DOI:10.3389/ti.2024.13495
Pierre Marquet, Dany Anglicheau, Antoine Humeau, Sofian Adrouche, Lakhdar Saada, Julie Bisiaux, Sara Guillemin, Audrey Lardy-Cléaud, Lionel Rostaing
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引用次数: 0

Abstract

All the factors potentially influencing tacrolimus dose requirement and combinations thereof have never been thoroughly investigated, precluding accurate prediction of tacrolimus starting dose. This prospective, non-interventional, multicenter study in de novo adult kidney transplant recipients over the first year after transplantation aimed to investigate the factors influencing tacrolimus dose-standardized trough blood concentration (C0/D) over the first week post-transplant (D4-D7, primary objective), D8-M3 and M3-M12 (secondary objectives). Statistical analysis employed mixed linear models with repeated measures. Eighteen sites enrolled 440 patients and followed them up for 9.5 ± 4.1 months. Age at baseline (p = 0.0144), end-stage renal disease (p = 0.0092), CYP3A phenotype (p < 0.0001), dyslipidemia at baseline (p = 0.0031), hematocrit (p = 0.0026), total bilirubin (p = 0.0261) and plasma creatinine (p = 0.0484) independently increased with log(C0/D) over D4-D7, explaining together 72.3% of the interindividual variability, and representing a robust model to estimate tacrolimus initial dose. Donor age and CYP3A phenotype were also influential over D8-M3 and M3-12, in addition to recipient age. Corticosteroids, diabetes at baseline, and ASAT yielded inconstant results between D8-M3 and M3-M12. We found no ethnicity effect when CYP3A phenotype was accounted for, and no food effect. Intra-individual variability over M3-M12 was moderate, and significantly lower in patients with chronic hepatic disorder (p = 0.0196) or cancer (p = 0.0132).

可以预测接受 Adoport® 治疗的新成人肾移植患者对他克莫司剂量的需求。
目前尚未对可能影响他克莫司剂量需求的所有因素及其组合进行深入研究,因此无法准确预测他克莫司的起始剂量。这项前瞻性、非干预性、多中心研究的目标是调查影响移植后第一周(D4-D7,首要目标)、D8-M3 和 M3-M12 (次要目标)他克莫司剂量标准化血槽浓度(C0/D)的因素。统计分析采用了重复测量混合线性模型。18 个研究机构共招募了 440 名患者,并对他们进行了 9.5 ± 4.1 个月的随访。基线年龄(p = 0.0144)、终末期肾病(p = 0.0092)、CYP3A 表型(p < 0.0001)、基线血脂异常(p = 0.0031)、血细胞比容(p = 0.0026)、总胆红素(p = 0.0261)和血浆肌酐(p = 0.0484)随 D4-D7 对数(C0/D)的增加而独立增加,共解释了 72.3% 的个体间变异,是估计他克莫司初始剂量的可靠模型。除受体年龄外,供体年龄和 CYP3A 表型对 D8-M3 和 M3-12 也有影响。皮质类固醇、基线糖尿病和 ASAT 在 D8-M3 和 M3-M12 之间产生的结果并不一致。当考虑到 CYP3A 表型时,我们没有发现种族效应,也没有发现食物效应。M3-M12 的个体内变异性适中,慢性肝病患者(p = 0.0196)或癌症患者(p = 0.0132)的个体内变异性明显较低。
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来源期刊
Transplant International
Transplant International 医学-外科
CiteScore
4.70
自引率
6.50%
发文量
211
审稿时长
3-8 weeks
期刊介绍: The aim of the journal is to serve as a forum for the exchange of scientific information in the form of original and high quality papers in the field of transplantation. Clinical and experimental studies, as well as editorials, letters to the editors, and, occasionally, reviews on the biology, physiology, and immunology of transplantation of tissues and organs, are published. Publishing time for the latter is approximately six months, provided major revisions are not needed. The journal is published in yearly volumes, each volume containing twelve issues. Papers submitted to the journal are subject to peer review.
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