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瑞马唑仑的临床药代动力学、药效学及药物相互作用

Clinical Pharmacokinetics, Pharmacodynamics, and Drug Interactions of Remimazolam.

作者信息

Murrell Derek E, Harirforoosh Sam

机构信息

Crown Laboratories, Johnson City, TN, USA.

Department of Biomedical and Pharmaceutical Sciences, School of Pharmacy, Chapman University, Irvine, CA, 92618, USA.

出版信息

Eur J Drug Metab Pharmacokinet. 2025 Sep 18. doi: 10.1007/s13318-025-00963-2.

DOI:10.1007/s13318-025-00963-2
PMID:40965620
Abstract

Remimazolam, an ultrashort-acting benzodiazepine, has emerged as a promising sedative agent for procedural sedation and general anesthesia. It combines the favorable properties of traditional benzodiazepines with a rapid onset and offset of action, largely due to its unique metabolism via hepatic carboxylesterases rather than cytochrome P450 enzymes. This metabolism allows for predictable pharmacokinetics, reducing the risk of prolonged sedation and drug accumulation, particularly in patients with hepatic or renal impairment. Clinically, remimazolam demonstrates non-inferiority to midazolam and propofol, with advantages including a lower incidence of hypotension and respiratory depression. Multiple randomized controlled trials have shown its efficacy in various procedural settings, including endoscopy and bronchoscopy, with high procedural success rates and faster recovery times compared to midazolam. Additionally, remimazolam is reversible with flumazenil, further enhancing its safety profile. Pharmacokinetic studies indicate a rapid distribution phase, a short terminal half-life of approximately 37-53 min, and a clearance rate significantly higher than midazolam. Pharmacodynamic analyses confirm dose-dependent sedation effects, making remimazolam suitable for tailored sedation levels across patient populations. Special population studies suggest minimal impact of age, renal function, or mild-to-moderate hepatic impairment on drug disposition. However, rare cases of anaphylaxis and re-sedation following flumazenil administration have been reported. Given its rapid onset, predictable clearance, and favorable safety profile, remimazolam represents a valuable alternative to existing sedatives in procedural and anesthetic applications. Further research is warranted to explore its long-term safety, expanded clinical applications, and potential role in high-risk populations.

摘要

瑞马唑仑是一种超短效苯二氮䓬类药物,已成为一种有前景的用于程序性镇静和全身麻醉的镇静剂。它结合了传统苯二氮䓬类药物的有利特性,起效和作用消失迅速,这主要归因于其通过肝脏羧酸酯酶而非细胞色素P450酶的独特代谢方式。这种代谢方式使得药代动力学具有可预测性,降低了长时间镇静和药物蓄积的风险,尤其是在肝肾功能不全的患者中。临床上,瑞马唑仑显示出与咪达唑仑和丙泊酚相当的效果,优点包括低血压和呼吸抑制的发生率较低。多项随机对照试验已表明其在包括内镜检查和支气管镜检查在内的各种程序性操作中的有效性,与咪达唑仑相比,具有较高的操作成功率和更快的恢复时间。此外,瑞马唑仑可用氟马西尼逆转,进一步提高了其安全性。药代动力学研究表明其分布相迅速,终末半衰期约为37 - 53分钟,清除率明显高于咪达唑仑。药效学分析证实了剂量依赖性镇静作用,使瑞马唑仑适用于不同患者群体的个体化镇静水平。特殊人群研究表明年龄、肾功能或轻度至中度肝功能损害对药物处置的影响最小。然而,已有报道称氟马西尼给药后出现罕见的过敏反应和再镇静病例。鉴于其起效迅速、清除可预测且安全性良好,瑞马唑仑在程序性操作和麻醉应用中是现有镇静剂的一种有价值的替代药物。有必要进一步研究其长期安全性、扩大临床应用范围以及在高危人群中的潜在作用。

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本文引用的文献

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Impact of genetic polymorphisms and drug-drug interactions mediated by carboxylesterase 1 on remimazolam deactivation.由羧酸酯酶1介导的基因多态性和药物-药物相互作用对瑞马唑仑失活的影响。
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Comparison of the anesthetic effects of remimazolam tosilate and remimazolam besylate in daytime hysteroscopic surgery.比较甲苯磺酸瑞马唑仑和甲磺酸瑞马唑仑在日间宫腔镜手术中的麻醉效果。
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Anesthesia management for percutaneous mitral valve repair in a patient with mitochondrial cardiomyopathy and low cardiac function: a case report.
线粒体心肌病伴心功能低下患者经皮二尖瓣修复术的麻醉管理:一例报告
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Carboxylesterase 1-Based Drug-Drug Interaction Potential of Remimazolam: Studies and Literature Review.基于羧酸酯酶 1 的雷米佐胺药物相互作用潜力:研究与文献综述。
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Incompatibility of the short-acting benzodiazepine remimazolam with common perioperative medication.短效苯二氮䓬类药物瑞马唑仑与常见围手术期用药不相容。
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