Apixaban dosing in hemodialysis - can drug level monitoring mitigate controversies?

IF 2.2 4区 医学 Q2 UROLOGY & NEPHROLOGY BMC Nephrology Pub Date : 2024-10-09 DOI:10.1186/s12882-024-03782-w
Simeon Schietzel, Andreas Limacher, Matthias B Moor, Cecilia Czerlau, Uyen Huynh-Do, Bruno Vogt, Fabienne Aregger, Dominik E Uehlinger
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Abstract

Background: Inconsistent study results and contradictory recommendations from health authorities regarding the use of apixaban in patients on hemodialysis have generated considerable uncertainty among clinicians, making investigations of appropriate dosing an unmet need.

Methods: We analyzed pre-dialysis apixaban drug levels from a tertiary care dialysis unit, comparing 2.5 mg once versus twice daily dosing. We applied mixed-effects models including dialysis modality, adjusted standard Kt/V, ultrafiltration, and dialyzer characteristics. We included an exploratory analysis of bleeding events and compared the drug levels of our dialysis patients to those from non-CKD reference populations taking the standard dose of 5 mg twice daily.

Results: We analyzed 143 drug levels from 24 patients. Mean (SD) age at first drug level measurement was 64.7 (15.9) years (50 % female), median (IQR) follow-up was 12.5 (5.5 - 21) months. For the apixaban 2.5 mg once and twice daily groups, median (IQR) drug levels were 54.4 (< 40 - 72.1) and 71.3 (48.8 - 104.1) ng/mL respectively (P < 0.001). Levels were below the detection limit in 30 % (with 2.5 mg once daily) and 14 % (with 2.5 mg twice daily) respectively. Only dosing group (twice versus once daily) was independently associated with higher drug levels (P = 0.002). Follow-up did not suggest accumulation. The 95th percentile of drug levels did not exceed those of non-CKD populations taking 5 mg twice daily. Median (IQR) drug levels before a bleeding (8 episodes) were higher than those without a subsequent bleeding: 111.6 (83.1 - 129.3) versus 54.8 (< 40 - 77.1) ng/mL (P < 0.001). Concomitant antiplatelet therapy was used in 86% of those with bleeding events versus 6% without bleeding events (P < 0.001).

Conclusions: Drug monitoring may be a contributory tool to increase patient safety. Despite non-existing target ranges, drug levels on both edges of the spectrum (e.g. below detectability or beyond the 95th percentiles of reference populations) may improve decision-making in highly individualized risk-benefit analyses.

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血液透析中的阿哌沙班剂量--药物浓度监测能否缓解争议?
背景:关于血液透析患者使用阿哌沙班的研究结果不一致,卫生部门的建议也相互矛盾,这给临床医生带来了很大的不确定性,因此对适当剂量的研究成为一项尚未满足的需求:我们分析了一家三级医疗透析单位透析前的阿哌沙班药物水平,比较了 2.5 毫克每日一次和每日两次的剂量。我们采用了混合效应模型,包括透析方式、调整后的标准 Kt/V、超滤和透析器特征。我们对出血事件进行了探索性分析,并将透析患者的药物水平与每日两次服用 5 毫克标准剂量的非 CKD 参考人群的药物水平进行了比较:我们分析了 24 名患者的 143 种药物水平。首次测量药物浓度时的平均(标清)年龄为 64.7(15.9)岁(50% 为女性),随访时间的中位数(IQR)为 12.5(5.5 - 21)个月。阿哌沙班 2.5 毫克每日一次组和每日两次组的药物浓度中位数(IQR)分别为 54.4(< 40 - 72.1)纳克/毫升和 71.3(48.8 - 104.1)纳克/毫升(P < 0.001)。药物水平低于检测限的比例分别为 30%(2.5 毫克,每天一次)和 14%(2.5 毫克,每天两次)。只有给药组别(每天两次与每天一次)与较高的药物浓度有独立关联(P = 0.002)。随访结果未显示药物蓄积。药物浓度的第 95 百分位数未超过每天两次、每次 5 毫克的非慢性阻塞性肺病患者。出血(8 次)前的药物浓度中位数(IQR)高于未发生出血的药物浓度中位数(IQR):111.6(83.1 - 129.3)纳克/毫升对 54.8(< 40 - 77.1)纳克/毫升(P < 0.001)。在发生出血事件的患者中,86%的患者同时使用了抗血小板疗法,而在未发生出血事件的患者中,只有6%的患者同时使用了抗血小板疗法(P < 0.001):结论:药物监测是提高患者安全性的有效工具。尽管不存在目标范围,但药物水平的两个边缘(如低于可检测水平或超过参考人群的第95百分位数)可改善高度个体化的风险-效益分析决策。
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来源期刊
BMC Nephrology
BMC Nephrology UROLOGY & NEPHROLOGY-
CiteScore
4.30
自引率
0.00%
发文量
375
审稿时长
3-8 weeks
期刊介绍: BMC Nephrology is an open access journal publishing original peer-reviewed research articles in all aspects of the prevention, diagnosis and management of kidney and associated disorders, as well as related molecular genetics, pathophysiology, and epidemiology.
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