Bevan_1994_Pharmacol.Toxicol_74_3

Reference

Title : Newer neuromuscular blocking agents - Bevan_1994_Pharmacol.Toxicol_74_3
Author(s) : Bevan DR
Ref : Pharmacol Toxicol , 74 :3 , 1994
Abstract :

Four neuromuscular blocking drugs, doxacurium, mivacurium, pipecuronium, and rocuronium have been or are about to be introduced into clinical practice. The purpose of this MiniReview is to describe their pharmacology, to consider their place in clinical anaesthetic practice, and to examine whether the needs of the clinician have been met. Two of the agents (doxacurium, mivacurium) are benzylisoquinolines resembling atracurium and two (pipecuronium, rocuronium) are aminosteroids related to pancuronium and vecuronium. Two (doxacurium, pipecuronium) are long-acting compounds, similar in duration of action to pancuronium, although the need for such a profile is questionable. Rocuronium has an intermediate duration of action and produces its maximum effect within two minutes which is much more rapid than any other non-depolarizing relaxant and this is probably a result of its poor potency. However, the onset of paralysis is not as quick as after succinylcholine. Mivacurium is unique because it is metabolized by plasma cholinesterase which produces a rapid recovery although slower than succinylcholine. All of the new drugs are devoid of serious cardiovascular or other side effects. The anaesthetist is now presented with an armamentarium of safe, nondepolarizing muscle relaxants with varying durations of action. However, the rapid onset and recovery associated with succinylcholine are unique and important in the urgent control of a patient's airway and respiration. The indications for succinylcholine will not disappear and the search for a non-polarizing replacement will continue.

PubMedSearch : Bevan_1994_Pharmacol.Toxicol_74_3
PubMedID: 8159634

Related information

Inhibitor Atracurium    Pipecuronium    Rocuronium    Doxacurium

Citations formats

Bevan DR (1994)
Newer neuromuscular blocking agents
Pharmacol Toxicol 74 :3

Bevan DR (1994)
Pharmacol Toxicol 74 :3