Abnormally high plasma concentrations of M-4, the active metabolite of edoxaban, at the onset of acute kidney injury in a patient receiving rifampin and clarithromycin: a case report.

IF 1.2 Q4 PHARMACOLOGY & PHARMACY Journal of Pharmaceutical Health Care and Sciences Pub Date : 2024-10-28 DOI:10.1186/s40780-024-00390-6
Junichi Nakagawa, Keinosuke Ishido, Norihisa Kimura, Hayato Nagase, Yusuke Wakasa, Satoshi Yokoyama, Kayo Ueno, Kenichi Hakamada, Takenori Niioka
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Abstract

Background: Edoxaban, the only factor Xa inhibitor with active metabolites, is metabolized by carboxylesterase-1 to its main active metabolite, M-4, which is a substrate of organic anion transporting polypeptide 1B1 (OATP1B1) and is excreted in bile and urine. Because the area under the plasma concentration-time curve ratio of M-4 to parent compound is typically less than 10% in healthy subjects, M-4 is generally considered to exhibit negligible antithrombotic activity in patients treated with edoxaban. However, we identified a case in which drug interactions and kidney impairment led to a substantive increase in plasma M-4 concentrations.

Case presentation: This case report involved a 68-year-old man with pancreatic cancer who was orally administered edoxaban tablets for prevention of thrombus formation in non-valvular atrial fibrillation, in addition to rifampin and clarithromycin (CAM) for treatment of mycobacterium avium complex lung disease. These medications were temporarily discontinued for a pancreaticoduodenectomy but were resumed 8 days post-surgery (POD8). On POD9, the patient developed acute kidney injury, and the trough concentrations of edoxaban and M-4 were 131.1 ng/mL and 115.8 ng/mL, respectively (M-4 ratio: 88.3%). On POD11, the M-4 trough concentration and M-4 ratio increased to 216.2 ng/mL and 186.2%, respectively. The plasma concentration of coproporphyrin-I, an endogenous biomarker of OATP1B1 activity, increased during this period.

Conclusions: This case suggests that in patients with impaired renal function taking edoxaban, co-administration of carboxylesterase-1 inducers such as rifampin and/or OATP1B1 inhibitors such as rifampin or clarithromycin may increase plasma concentrations of M-4 to clinically non-negligible levels.

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在一名接受利福平和克拉霉素治疗的患者急性肾损伤发病时,其血浆中艾多沙班的活性代谢产物 M-4 浓度异常高:一份病例报告。
背景:埃多沙班是唯一具有活性代谢物的Xa因子抑制剂,通过羧基酯酶-1代谢为主要活性代谢物M-4,M-4是有机阴离子转运多肽1B1(OATP1B1)的底物,通过胆汁和尿液排出体外。由于在健康受试者中,M-4 与母体化合物的血浆浓度-时间曲线下面积比通常低于 10%,因此一般认为 M-4 在接受埃多沙班治疗的患者中表现出的抗血栓活性可以忽略不计。然而,我们发现了一例药物相互作用和肾功能损害导致血浆中 M-4 浓度大幅升高的病例:本病例报告涉及一名患有胰腺癌的 68 岁男性患者,他在口服埃多沙班片预防非瓣膜性心房颤动血栓形成的同时,还口服利福平和克拉霉素(CAM)治疗复合肺分枝杆菌病。这些药物因胰十二指肠切除术而暂时停用,但在术后 8 天(POD8)恢复使用。POD9 日,患者出现急性肾损伤,埃多沙班和 M-4 的谷浓度分别为 131.1 纳克/毫升和 115.8 纳克/毫升(M-4 比率:88.3%)。在 POD11,M-4 谷浓度和 M-4 比率分别增至 216.2 纳克/毫升和 186.2%。在此期间,OATP1B1活性的内源性生物标志物共卟啉-I的血浆浓度也有所上升:本病例表明,在肾功能受损的患者服用埃多沙班时,同时服用羧酸酯酶-1诱导剂(如利福平)和/或OATP1B1抑制剂(如利福平或克拉霉素)可能会使血浆中的M-4浓度升高至临床上不可忽略的水平。
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来源期刊
CiteScore
1.80
自引率
0.00%
发文量
29
审稿时长
8 weeks
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