Profiling metoprolol enantiomers in urine of hypertensive patients.

IF 2.1 4区医学 Q3 PHARMACOLOGY & PHARMACY

DARU Journal of Pharmaceutical Sciences Pub Date : 2025-07-03 DOI:10.1007/s40199-025-00563-0

Behrouz Seyfinejad, Kimiya Jouyban, Jalil Houshyar, Amirreza Jabbaripour Sarmadian, Abolghasem Jouyban

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Abstract

Background: Metoprolol, a widely used β-blocker, is administered as a racemic mixture, with (S)-metoprolol being more pharmacologically active. Its metabolism by CYP2D6 exhibits significant inter-individual variability due to genetic polymorphisms. While enantioselective pharmacokinetics have been studied in single-dose trials, data on long-term therapy in hypertensive patients is limited. This study examines urinary enantiomer profiles to assess variability in metabolism and excretion.

Objectives: This study investigates the enantiomeric profile of metoprolol in urine samples collected from hypertensive patients receiving long-term racemic metoprolol therapy. The research aims to improve the analytical performance of the method to explore the enantioselective metabolism and excretion of the drug, focusing on the variation in enantiomer ratios among patients and the potential implications for clinical practice.

Methods: Urine samples were collected from 30 hypertensive patients treated with racemic metoprolol. The samples were analyzed using capillary electrophoresis (CE) with clarithromycin as a chiral selector. Prior to CE analysis, liquid-liquid extraction was performed to isolate metoprolol from urine. The CE method employed an online preconcentration method and had a detection limit of 0.015 µg mL^-1 for each enantiomer, a linear range of 0.05 to 2.0 µg mL^-1, and demonstrated intra-day and inter-day precision below 6.3%, with accuracy within 5.6%.

Results: Metoprolol enantiomers were quantified in patients' urine samples, with enantiomer ratios varying among individuals. The enantiomer ratio (S/R) exceeded 1 in most patients, reflecting higher (S)-metoprolol concentrations. However, in approximately 40% of patients, the ratio was less than 1, suggesting possible enantioselective renal excretion.

Conclusion: The study confirms that there is substantial inter-individual variability in the enantioselective metabolism and excretion of metoprolol among hypertensive patients. The findings emphasize the need to consider enantioselective pharmacokinetics in clinical practice, especially for chiral drugs like metoprolol. The results also suggest that the duration of treatment may affect the metabolism and excretion of enantiomers, warranting further investigation into the effects of long-term drug administration on enantiomeric ratios.

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高血压患者尿中美托洛尔对映体的分析。

背景：美托洛尔是一种广泛使用的β受体阻滞剂，以外消旋混合物的形式给药，其中(S)-美托洛尔具有更强的药理活性。由于遗传多态性，CYP2D6对其代谢表现出显著的个体间差异。虽然单剂量试验研究了对映体选择性药代动力学，但高血压患者长期治疗的数据有限。本研究检查尿液对映体的概况，以评估代谢和排泄的变异性。目的：研究长期接受外消旋美托洛尔治疗的高血压患者尿液样本中美托洛尔的对映体特征。本研究旨在提高该方法的分析性能，以探索药物的对映体选择性代谢和排泄，重点关注患者对映体比例的变化及其对临床实践的潜在影响。方法：收集30例接受外消旋美托洛尔治疗的高血压患者尿液。以克拉霉素为手性选择剂，采用毛细管电泳（CE）对样品进行分析。在进行CE分析之前，采用液-液萃取法从尿液中分离美托洛尔。CE法采用在线预富集法，各对映体的检出限为0.015µg mL-1，线性范围为0.05 ~ 2.0µg mL-1，日内、日间精密度均在6.3%以下，准确度在5.6%以内。结果：对患者尿液样本中的美托洛尔对映体进行了量化，个体间对映体比例不同。大多数患者的对映体比（S/R）超过1，反映了较高的(S)-美托洛尔浓度。然而，在大约40%的患者中，该比值小于1，提示可能存在对映选择性肾排泄。结论：本研究证实高血压患者美托洛尔的对映选择性代谢和排泄存在显著的个体差异。研究结果强调了在临床实践中考虑对映体选择性药代动力学的必要性，特别是对于像美托洛尔这样的手性药物。结果还表明，治疗时间可能会影响对映体的代谢和排泄，需要进一步研究长期给药对对映体比例的影响。

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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DARU Journal of Pharmaceutical Sciences PHARMACOLOGY & PHARMACY-

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期刊介绍： DARU Journal of Pharmaceutical Sciences is a peer-reviewed journal published on behalf of Tehran University of Medical Sciences. The journal encompasses all fields of the pharmaceutical sciences and presents timely research on all areas of drug conception, design, manufacture, classification and assessment. The term DARU is derived from the Persian name meaning drug or medicine. This journal is a unique platform to improve the knowledge of researchers and scientists by publishing novel articles including basic and clinical investigations from members of the global scientific community in the forms of original articles, systematic or narrative reviews, meta-analyses, letters, and short communications.