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在广泛和中等 CYP3A5 代谢人群中,肾移植受者需要更多的他克莫司剂量调整。

Higher number of tacrolimus dose adjustments in kidney transplant recipients who are extensive and intermediate CYP3A5 metabolizers.

机构信息

Department of Pharmacy, Hennepin County Medical Center, Minneapolis, Minnesota, USA.

Hennepin Healthcare Research Institute, Minneapolis, Minnesota, USA.

出版信息

Clin Transplant. 2023 Apr;37(4):e14893. doi: 10.1111/ctr.14893. Epub 2023 Jan 11.

Abstract

Kidney transplant recipients carrying the CYP3A51 allele have lower tacrolimus troughs, and higher dose requirements compared to those with the CYP3A53/*3 genotype. However, data on the effect of CYP3A5 alleles on post-transplant tacrolimus management are lacking. The effect of CYP3A5 metabolism phenotypes on the number of tacrolimus dose adjustments and troughs in the first 6 months post-transplant was evaluated in 78 recipients (64% Caucasians). Time to first therapeutic concentration, percentage of time in therapeutic range (TTR), and estimated glomerular filtration rate (eGFR) were also evaluated. Fifty-five kidney transplant recipients were CYP3A5 poor metabolizers (PM), 17 were intermediate metabolizers (IM), and 6 were extensive metabolizers (EM). Compared to PMs, EMs/IMs had significantly more dose adjustments (6.1 vs. 8.1, p = .015). Overall, 33.82% of trough measurements resulted in a dose change. There was no difference in the number of tacrolimus trough measurements between PMs and EM/IMs. The total daily tacrolimus dose requirements were higher in EMs and IMs compared to PMs (<.001). TTR was ∼50% in the PMs and EMs/IMs groups. CYP3A5 EM/IM metabolizers have more tacrolimus dose changes and higher dose requirements which increases clinical management complexity. Larger studies are needed to assess the cost and benefits of including genotyping data to improve clinical management.

摘要

携带 CYP3A51 等位基因的肾移植受者的他克莫司谷浓度较低,与 CYP3A53/*3 基因型的受者相比,需要更高的剂量。然而,关于 CYP3A5 等位基因对移植后他克莫司管理影响的数据尚缺乏。本研究评估了 CYP3A5 代谢表型对 78 例肾移植受者(64%为白种人)移植后 6 个月内他克莫司剂量调整和谷浓度的影响。还评估了首次治疗浓度时间、治疗浓度范围内的时间百分比(TTR)和估算肾小球滤过率(eGFR)。55 例肾移植受者为 CYP3A5 弱代谢者(PM),17 例为中间代谢者(IM),6 例为广泛代谢者(EM)。与 PM 相比,EM/IM 有更多的剂量调整(6.1 比 8.1,p = 0.015)。总体而言,33.82%的谷浓度测量值导致剂量改变。PM 和 EM/IM 之间的他克莫司谷浓度测量值没有差异。与 PM 相比,EM 和 IM 的他克莫司总日剂量要求更高(<0.001)。PM 和 EM/IM 组的 TTR 约为 50%。CYP3A5 强代谢者有更多的他克莫司剂量变化和更高的剂量要求,这增加了临床管理的复杂性。需要更大的研究来评估包括基因分型数据以改善临床管理的成本和效益。

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