Pharmacokinetics, Tolerability, and Safety of Esmethadone in Subjects with Chronic Kidney Disease or Hepatic Impairment.

IF 2.2 4区医学 Q3 PHARMACOLOGY & PHARMACY

Drugs in Research & Development Pub Date : 2024-06-01 Epub Date: 2024-08-03 DOI:10.1007/s40268-024-00477-3

Nicola Ferri, Sara De Martin, James Stuart, Sergio Traversa, Andrea Mattarei, Stefano Comai, Franco Folli, Marco Pappagallo, Clotilde Guidetti, Charles E Inturrisi, Paolo L Manfredi

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Abstract

Background and objectives: Esmethadone (dextromethadone; d-methadone; S-methadone (+)-methadone; REL-1017) is a low potency N-methyl-_D-aspartate (NMDA) receptor channel blocker that showed a rapid and sustained adjunctive antidepressant effects in patients with major depressive disorder with inadequate response to ongoing serotonergic antidepressant treatment. Previous studies indicated that esmethadone is partially excreted by the kidney (53.9% of the dose) and by the liver (39.1% of the dose).

Methods: Here we studied the pharmacokinetics and safety of esmethadone after a single oral dose of 25 mg in subjects with different stages of kidney and liver impairment.

Results: In subjects with a mild and moderate decrease in glomerular fraction rate (GFR), esmethadone C_max and AUC_0-inf values did not differ compared with healthy subjects. In patients with severe renal impairment, the ratios of C_max and AUC_0-inf values compared with healthy subjects were above 100% (138.22-176.85%) and, while modest, these increases reached statistical significance. In subjects with end stage renal disease (ESRD) undergoing intermittent hemodialysis (IHD), C_max and AUC_0-inf values were not statistically different compared with healthy subjects. IHD did not modified plasma total esmethadone concentrations in blood exiting versus entering the dialyzer. Dose adjustment is not warranted in subjects with mild-to-moderate impaired renal function. Dose reduction may be considered for select patients with severe renal disfunction. In subjects with mild-or-moderate hepatic impairment, C_max and AUC_0-inf were approximately 20-30% lower compared with healthy controls. The drug free fraction increased with the severity of hepatic impairment, from 5.4% in healthy controls to 8.3% in subjects with moderate hepatic impairment.

Conclusion: Mild and moderate hepatic impairment has a minimal to modest impact on exposure to total or unbound esmethadone and dose adjustments are not warranted in subjects with mild and moderate hepatic impairment. Administration of esmethadone was well tolerated in healthy adult subjects, in subjects with mild or moderate hepatic impairment, and in subjects with mild moderate or severe renal impairment, including patients with ESRF undergoing dialysis.

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慢性肾病或肝功能不全患者服用艾司美沙酮的药代动力学、耐受性和安全性

背景和目的：艾司美沙酮（右旋美沙酮；d-美沙酮；S-美沙酮(+)-美沙酮；REL-1017）是一种低效的N-甲基-D-天冬氨酸（NMDA）受体通道阻断剂，对正在接受血清素能抗抑郁剂治疗但反应不充分的重度抑郁症患者具有快速、持续的辅助抗抑郁作用。以前的研究表明，艾司美沙酮部分通过肾脏排泄（占剂量的53.9%），部分通过肝脏排泄（占剂量的39.1%）。方法：我们在此研究了不同阶段肝肾功能受损的受试者单次口服25毫克艾司美沙酮后的药代动力学和安全性：结果：在肾小球滤过率（GFR）轻度和中度下降的受试者中，艾司美沙酮的Cmax和AUC0-inf值与健康受试者相比没有差异。在重度肾功能损害患者中，与健康受试者相比，其 Cmax 和 AUC0-inf 值的比率高于 100%（138.22%-176.85%），尽管比率不高，但这些增加具有统计学意义。在接受间歇性血液透析（IHD）的终末期肾病（ESRD）受试者中，Cmax 和 AUC0-inf 值与健康受试者相比没有统计学差异。间歇性血液透析（IHD）不会改变血液流出和进入透析器时血浆中的艾司美沙酮总浓度。肾功能轻度至中度受损的受试者无需调整剂量。部分肾功能严重受损的患者可考虑减少剂量。与健康对照组相比，轻度或中度肝功能损害受试者的 Cmax 和 AUC0-inf 降低约 20-30%。药物游离部分随肝功能损害的严重程度而增加，从健康对照组的 5.4% 增加到中度肝功能损害受试者的 8.3%：结论：轻度和中度肝功能损害对总的或未结合的艾司美沙酮的暴露量影响很小，无需对轻度和中度肝功能损害的受试者进行剂量调整。健康成年受试者、轻度或中度肝功能损害受试者以及轻度、中度或重度肾功能损害受试者（包括正在进行透析的ESRF患者）对服用艾司美沙酮的耐受性良好。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Drugs in Research & Development Pharmacology, Toxicology and Pharmaceutics-Pharmacology

CiteScore

5.10

自引率

0.00%

发文量

审稿时长

8 weeks

期刊介绍： Drugs in R&D is an international, peer reviewed, open access, online only journal, and provides timely information from all phases of drug research and development that will inform clinical practice. Healthcare decision makers are thus provided with knowledge about the developing place of a drug in therapy. The Journal includes: Clinical research on new and established drugs; Preclinical research of direct relevance to clinical drug development; Short communications and case study reports that meet the above criteria will also be considered; Reviews may also be considered.