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神经肌肉阻滞的逆转。

Reversal of neuromuscular block.

作者信息

Srivastava A, Hunter J M

机构信息

University of Liverpool Critical Care Research Unit, School of Clinical Science, Daulby Street, Liverpool, UK.

出版信息

Br J Anaesth. 2009 Jul;103(1):115-29. doi: 10.1093/bja/aep093. Epub 2009 May 24.

DOI:10.1093/bja/aep093
PMID:19468024
Abstract

The use of anticholinesterases to reverse residual neuromuscular block is efficacious only if recovery is already established. It was originally advised that at least the second twitch (T2) of the train-of-four response should be detectable before neostigmine is administered. Even in these circumstances, the full effect of anticholinesterases takes up to 10 min to achieve. Anticholinesterases also have muscarinic side-effects that require an antimuscarinic to be administered concomitantly. An ideal reversal agent could be given at any time after the administration of a neuromuscular blocking agent (NMBA), and should have no muscarinic side-effects. The gamma cyclodextrin, sugammadex, has been demonstrated to effectively antagonize even profound block produced by the aminosteroid NMBAs, rocuronium and vecuronium, by chelating them. The complex is then excreted in the urine. Sugammadex is ineffective in antagonizing the benzylisoquinolinium NMBAs. The dose should be adjusted according to the degree of residual block: sugammadex 16 mg kg(-1) for immediate reversal; 4-8 mg kg(-1) for antagonizing profound block (post-tetanic count 1-2); and 2 mg kg(-1) to antagonize moderate block (when T2 is detectable). As yet, the extent of any side-effects that may occur with this new antagonist is not fully known, although rarely adverse cardiovascular effects (hypotension, hypertension, prolonged QT interval) have already been reported.

摘要

仅当神经肌肉功能已开始恢复时,使用抗胆碱酯酶药来逆转残余的神经肌肉阻滞才有效。最初建议在给予新斯的明之前,四个成串刺激反应中至少应能检测到第二个肌颤搐(T2)。即便如此,抗胆碱酯酶药的全部作用仍需长达10分钟才能显现。抗胆碱酯酶药还会产生毒蕈碱样副作用,因此需要同时给予抗毒蕈碱药。理想的逆转剂应能在给予神经肌肉阻滞药(NMBA)后的任何时间使用,且不应有毒蕈碱样副作用。γ-环糊精舒更葡糖已被证明可通过螯合作用有效拮抗甾体类NMBA罗库溴铵和维库溴铵所致的深度阻滞。形成的复合物随后经尿液排出。舒更葡糖对苄异喹啉类NMBA无效。剂量应根据残余阻滞的程度进行调整:立即逆转时舒更葡糖剂量为16 mg·kg⁻¹;拮抗深度阻滞(强直刺激后计数为1 - 2)时为4 - 8 mg·kg⁻¹;拮抗中度阻滞(T2可检测到时)为2 mg·kg⁻¹。尽管已有报道称偶尔会出现不良心血管效应(低血压、高血压、QT间期延长),但目前尚不完全清楚这种新型拮抗剂可能产生的副作用程度。

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