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Transcript
Neuromuscular Blockade Suzanne Wake NEMSA SpR September 2008 Objective Safe use of Neuromuscular Blockade Contents • Physiology of neuromuscular junction (NMJ) • Pharmacology of commonly used neuromuscular blocking drugs (NMBDs) • Monitoring neuromuscular blockade (MNB) Physiology - Structure of NMJ • NMJ consists of – Pre-synaptic motor neurone – Synaptic cleft (20nm) – Motor end plate ie post-synaptic membrane of striated muscle cell, rich in acetylcholine receptors (Ach-r) Structure of NMJ Physiology - Acetylcholine • Synthesised in presynaptic neurone • Nerve stimulus release into synaptic cleft • Binds to post-synaptic Ach-r • Hydrolysed by Acetylcholinesterase (Ach-E) Physiology – Acetylcholine Receptor • Nicotinic • Pentameric cylinder • 2 a sub-units = 2 Ach binding sites • Transmembrane • Central ion channel • Ach binding conformation change channel opens a a Pharmacology - Structure of NMBDs • Quaternary ammonium compounds related to Ach Pharmacology–Classification of NMBDs • Depolarising NMBDs • Non-depolarising NMBDs Depolarising NMBDs • Ach-r agonists • Succinylcholine Succinylcholine • Binds to Ach-r causing – Membrane depolarisation – Prolonged activation of Ach-r – Muscle flaccidity (<60s) • Phase 1 (Accomodation) Block • Recovery as drug diffuses away (3-15 mins) • Metabolised by plasma cholinesterase Side Effects of Succinylcholine LETHAL NON-LETHAL Anaphylaxis Bradycardia intraocular intracranial intragastric pressure Myalgia Prolonged action (pCh deficiency) Myotonia contracture Arrest (muscarinic effect) Hyperkalaemia MH trigger Non-Depolarising NMBDs • Competitive, reversible antagonists at postsynaptic Ach-r • 75% Ach-r block for loss of contraction • Benzolisoquinoliniums (--curium) • Aminosteroids (--curonium) Benzolisoquinolonium Compounds • Histamine release • Atracurium – Hofmann degradation (45%) – Ester hydrolysis • Mivacurium – Short acting – Hydrolysed by plasma cholinesterases Aminosteroid Compounds • No histamine release • Depend on organ function for excretion • Rocuronium – Rapid onset – Hepatic excretion – Anaphylactoid rxns more common Ideal NMBD • • • • • • • • Nondepolarising Rapid onset/offset Reversible with AchE No histamine release No CVS effects Non-cumulative No drug interactions No organ toxicity or excretion Monitoring NMB – Why? • • • • Timing of tracheal intubation Intra-operative muscle relaxation Reversal of NMB Timing of tracheal extubation Monitoring NMB – How? • • • • Supra-maximal stimulus (15-60mA) Elicit whole muscle response Square wave stimulus Duration < refractory period of NMJ Patterns of Stimulation • • • • Single Twitch Train of Four (TOF) Tetany Double Burst Stimulation Single Twitch • 0.1-1Hz • Requires control measurement (T1/Tc) • Depolarising block 100% Tc T1 T2 T3 T4 Train of Four • • • • • 2Hz Nondepolarising block TOF ratio (T4/T1) Fade (presynaptic Ach-r block) T4/T1>0.9 for safe extubation 100% T1 T2 T3 T4 Tetany • 50-100Hz for 5s • Nondepolarising and phase 2 block show fade • Post Tetanic Facilitation – 50Hz for 5s, 3s pause, 1Hz single stimuli – Used in profound nondepolarising NMB Double Burst Stimulation • 3, 50Hz twitches, 750ms pause, repeat • Improves manual detection of fade – Perceived at TOF ratio 0.6 cf 0.4 Summary Reversal of NMB • Neostigmine PLUS • Antimuscarinic OR • Sugamadex (the future)
