Department of Medicine Solna, Karolinska Institutet & Clinical Pharmacology, Karolinska University Hospital, Stockholm, Sweden.
Department of Clinical Sciences, Karolinska Institutet & Division of Cardiovascular Medicine, Danderyd Hospital, Stockholm, Sweden.
Biomed Pharmacother. 2024 Nov;180:117613. doi: 10.1016/j.biopha.2024.117613. Epub 2024 Oct 28.
The direct factor Xa inhibitor apixaban is partially eliminated by the kidneys but is still prescribed at fixed doses without therapeutic drug monitoring across varying levels of renal function. If apixaban accumulates due to renal impairment, this may translate into safety concerns, e.g. the risk for bleeding. The purpose of this study was to measure apixaban trough concentrations in patients with different stages of renal function/renal impairment.
Apixaban trough concentrations were measured using LC-MS/MS in patients with atrial fibrillation, having normal renal function (apixaban 5 mg BID, n=39), moderate renal impairment (apixaban 5 mg BID, n=40) and severe renal impairment (apixaban 2.5 mg BID, n=6). The median (min-max) relative eGFR values were 84.8 (71.7-111.4), 51.4 (31.3-67.2) and 23.0 (21.9-28.4) mL/min/1.73 m², in the three groups, respectively.
Patients with moderate renal impairment had significantly higher apixaban trough concentrations than patients with normal renal function. The median (min-max) trough concentrations were 59.8 ng/mL (15.5-170.9) for normal renal function, 128.9 ng/mL (41.4-295.4) for moderate renal impairment and 81.7 ng/mL (61.8-109.0) for severe renal impairment. The trough concentrations correlated significantly with renal function measured as relative/absolute eGFR creatinine/cystatin C.
The standard dosing regimen of 5 mg apixaban BID renders exposure that is roughly twice as high in patients with moderately reduced renal function compared to patients with normal renal function. We suggest that patients with moderately reduced renal function ought to be monitored. Possibly, a dose reduction may be considered to achieve similar exposure as in patients with normal renal function.
直接因子 Xa 抑制剂阿哌沙班部分经肾脏消除,但在不同肾功能水平下仍按固定剂量开处方,而无需进行治疗药物监测。如果阿哌沙班因肾功能损害而蓄积,则可能会出现安全性问题,例如出血风险。本研究旨在测量不同肾功能/肾功能不全阶段患者的阿哌沙班谷浓度。
使用 LC-MS/MS 测量了 39 名具有正常肾功能(阿哌沙班 5mg BID)、40 名中度肾功能不全(阿哌沙班 5mg BID)和 6 名严重肾功能不全(阿哌沙班 2.5mg BID)的心房颤动患者的阿哌沙班谷浓度。三组患者的中位(最小-最大)相对 eGFR 值分别为 84.8(71.7-111.4)、51.4(31.3-67.2)和 23.0(21.9-28.4)mL/min/1.73m²。
中度肾功能不全患者的阿哌沙班谷浓度明显高于正常肾功能患者。正常肾功能组的中位(最小-最大)谷浓度为 59.8ng/mL(15.5-170.9),中度肾功能不全组为 128.9ng/mL(41.4-295.4),严重肾功能不全组为 81.7ng/mL(61.8-109.0)。谷浓度与相对/绝对 eGFR 肌酐/胱抑素 C 测量的肾功能显著相关。
标准剂量 5mg 阿哌沙班 BID 使肾功能中度降低的患者的暴露量大约是正常肾功能患者的两倍。我们建议对肾功能中度降低的患者进行监测。可能需要考虑减少剂量以达到与正常肾功能患者相似的暴露量。
