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危重症中常用神经肌肉阻滞剂的应用药理学

Applied pharmacology of common neuromuscular blocking agents in critical care.

作者信息

Prielipp R C, Coursin D B

机构信息

Department of Anesthesiology, University of Wisconsin Clinical Science Center, Madison 53792-3272.

出版信息

New Horiz. 1994 Feb;2(1):34-47.

PMID:7922428
Abstract

While all neuromuscular blocking agents (NMBAs) effectively interrupt neuromuscular transmission, it must be emphasized that these drugs are completely devoid of analgesic, sedative, or amnestic properties. The increasing use of NMBAs in the ICU requires familiarity with their basic pharmacologic properties, as well as an appreciation of potential problems associated with chronic (> 24 hrs) neuromuscular blockade. Although NMBAs possess an impressive safety record, the majority of recommendations for neuromuscular blocker use in the ICU are extrapolated from short-term perioperative studies in healthy patients. NMBAs are structurally related to acetylcholine and their main site of action is the postjunctional nicotinic acetylcholine receptor, although prejunctional interaction may be an important component of total activity. These drugs act to either sustain a depolarization at the postjunctional membrane (succinylcholine), or they inhibit neuromuscular transmission by a competitive (non-depolarizing) blocking mechanism. Adverse hemodynamic consequences may result from concurrent stimulation of muscarinic receptors, autonomic ganglia, histamine, or catecholamine release associated with some agents. The metabolism and excretion of NMBAs may be altered in ICU patients with end-organ dysfunction, concurrent medications, electrolyte, acid-base, and nutritional abnormalities, along with underlying nervous system and muscle pathology. Prolonged weakness after discontinuation of NMBAs is increasingly recognized after these agents are used for extended periods. This phenomenon may be related to alterations in the pharmacokinetics and pharmacodynamics, along with altered physiology of the neuromuscular junction, nervous system, or muscle, or other undefined toxic effects. A sound knowledge of the basic physiology of the neuromuscular junction, neuromuscular blocker pharmacology, and standard techniques to assess the degree of neuromuscular blockade provides the rationale for drug selection when paralysis is indicated in ICU patients.

摘要

虽然所有神经肌肉阻滞剂(NMBA)都能有效中断神经肌肉传递,但必须强调的是,这些药物完全没有镇痛、镇静或遗忘作用。重症监护病房(ICU)中NMBA的使用日益增多,这就要求熟悉其基本药理特性,并了解与慢性(>24小时)神经肌肉阻滞相关的潜在问题。尽管NMBA有着令人印象深刻的安全记录,但ICU中使用神经肌肉阻滞剂的大多数建议都是从健康患者的短期围手术期研究中推断出来的。NMBA在结构上与乙酰胆碱相关,其主要作用部位是接头后烟碱型乙酰胆碱受体,尽管接头前相互作用可能是总活性的重要组成部分。这些药物的作用要么是在接头后膜维持去极化(琥珀酰胆碱),要么是通过竞争性(非去极化)阻断机制抑制神经肌肉传递。某些药物相关的毒蕈碱受体、自主神经节、组胺或儿茶酚胺释放的同时刺激可能导致不良血流动力学后果。在患有终末器官功能障碍、同时使用多种药物、存在电解质酸碱和营养异常以及潜在神经系统和肌肉病变的ICU患者中,NMBA的代谢和排泄可能会发生改变。在这些药物长期使用后,停药后出现的肌无力持续时间延长越来越受到关注。这种现象可能与药代动力学和药效学的改变、神经肌肉接头、神经系统或肌肉的生理改变或其他未明确的毒性作用有关。了解神经肌肉接头的基本生理学、神经肌肉阻滞剂药理学以及评估神经肌肉阻滞程度的标准技术,为ICU患者需要麻痹时的药物选择提供了理论依据。

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