Literature DB >> 9989341

Clinical pharmacokinetics of cisatracurium besilate.

D F Kisor1, V D Schmith.   

Abstract

Cisatracurium besilate, one of the 10 stereoisomers that comprise atracurium besilate, is a nondepolarising neuromuscular blocking agent with an intermediate duration of action. Following a 5- to 10-sec intravenous bolus dose of cisatracurium besilate to healthy young adult surgical patients, elderly patients and patients with renal or hepatic failure, the concentration versus time profile of cisatracurium besilate is best characterised by a 2-compartment model. The volume of distribution (Vd) of cisatracurium besilate is small because of its relatively large molecular weight and high polarity. Cisatracurium besilate undergoes Hofmann elimination, a process dependent on pH and temperature. Unlike atracurium besilate, cisatracurium besilate does not appear to be degraded directly by ester hydrolysis. Hofmann elimination, an organ independent elimination pathway, occurs in plasma and tissue, and is responsible for approximately 77% of the overall elimination of cisatracurium besilate. The total body clearance (CL), steady-state Vd and elimination half-life of cisatracurium besilate in patients with normal organ function are approximately 0.28 L/h/kg (4.7 ml/min/kg), 0.145 L/kg and 25 minutes, respectively. The magnitude of interpatient variability in the CL of cisatracurium besilate is low (16%), a finding consistent with the strict physiological control of the factors that effect the Hofmann elimination of cisatracurium besilate (i.e. temperature and pH). There is a unique relationship between plasma clearance and Vd because the primary elimination pathway for cisatracurium besilate is not dependent on organ function. There are minor differences in the pharmacokinetics of cisatracurium besilate in various patient populations. These differences are not associated with clinically significant differences in the recovery profile of cisatracurium besilate, but may be associated with differences in the time to onset of neuromuscular block.

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Year:  1999        PMID: 9989341     DOI: 10.2165/00003088-199936010-00003

Source DB:  PubMed          Journal:  Clin Pharmacokinet        ISSN: 0312-5963            Impact factor:   6.447


  37 in total

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  15 in total

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Review 2.  Use of neuromuscular blocking agents in acute respiratory distress syndrome.

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3.  The pharmacokinetics and pharmacodynamics of cisatracurium in critically ill patients with severe sepsis.

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4.  Pharmacokinetic/Pharmacodynamic Model of CW002, an Investigational Intermediate Neuromuscular Blocking Agent, in Healthy Volunteers.

Authors:  Josh D Kaullen; Joel S Owen; Kim L R Brouwer; Paul M Heerdt; Cynthia A Lien; John J Savarese; Virginia D Schmith
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5.  Atracurium during induced hyperthermia.

Authors:  Gersten Jonker; Leo J Hoogenboom; Bert van Ramshorst; Peter Bruins
Journal:  J Anesth       Date:  2009-08-14       Impact factor: 2.078

6.  Effect of nitrous oxide on cisatracurium infusion demands: a randomized controlled trial.

Authors:  Hanna L Illman; Heikki Mj Antila; Klaus T Olkkola
Journal:  BMC Anesthesiol       Date:  2010-08-18       Impact factor: 2.217

7.  Cisatracurium degradation: Intravenous fluid warmer the culprit?

Authors:  Rashid M Khan; Naresh Kaul; Raj Gopal Nair
Journal:  Indian J Anaesth       Date:  2015-05

8.  Cellular exposure to muscle relaxants and propofol could lead to genomic instability in vitro.

Authors:  Allen Edward Coleman; Nicole McNeil; Alexander Leonidovich Kovalchuck; Dara Wangsa; Thomas Ried; Hong Wang
Journal:  J Biomed Res       Date:  2012-03

9.  The effect of low dose ketamine and priming of cisatracurium on the intubating condition and onset time of cisatracurium.

Authors:  Byung-Ryang Ahn; Sang-Hun Kim; Byung-Sik Yu; Kyung-Joon Lim; Jong-June Sun
Journal:  Korean J Anesthesiol       Date:  2012-10-12

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Authors:  Feng Xiaobo; Ke Jianjuan; Wang Yanlin
Journal:  Braz J Med Biol Res       Date:  2012-05-17       Impact factor: 2.590

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