Temperature-dependent Pharmacokinetics and Pharmacodynamics of Vecuronium

Author:

Caldwell James E.1,Heier Tom2,Wright Peter M. C.3,Lin Sean4,McCarthy Gerald5,Szenohradszky Janos6,Sharma Manohar L.7,Hing Jeremy P.8,Schroeder Marc4,Sessler Daniel I.9

Affiliation:

1. Professor of Anesthesia, University of California–San Francisco.

2. Assistant Professor of Anesthesia, University of California–San Francisco. Current position: Consultant Anesthetist, Ullevaal University, Oslo, Norway.

3. Senior Lecturer, University of Newcastle-upon-Tyne, Newcastle-upon-Tyne, United Kingdom.

4. Research Associate, University of California–San Francisco.

5. Assistant Professor of Anesthesia, University of California–San Francisco. Current position: Consultant Anesthetist, The Queens University of Belfast, Belfast, United Kingdom.

6. Assistant Professor of Anesthesia, University of California–San Francisco. Current position: Assistant Professor of Anesthesia, University of Southern California, Los Angeles, California.

7. Research Chemist, University of California–San Francisco.

8. Research Associate, University of Newcastle-upon-Tyne, Newcastle-upon-Tyne, United Kingdom.

9. Professor of Anesthesia, University of California–San Francisco; Professor, Ludwig Boltzmann Institute for Clinical Anesthesia and Intensive Care, Vienna, Austria; Director, Outcomes Research™, and Vice Chair, Department of Anesthesia and General Intensive Care, University of Vienna, Vienna, Austria.

Abstract

Background The authors evaluated the influence of temperature on the pharmacokinetics and pharmacodynamics of vecuronium because mild core hypothermia doubles its duration of action. Methods Anesthesia was induced with alfentanil and propofol and maintained with nitrous oxide and isoflurane in 12 healthy volunteers. Train-of-four stimuli were applied to the ulnar nerve, and the mechanical response of the adductor pollicis was measured. Volunteers were actively cooled or warmed until their distal esophageal temperatures were in one of four ranges: < 35.0 degrees C, 35.0-35.9 degrees C, 36.0-36.9 degrees C, and > or = 37.0 degrees C. With temperature stabilized, vecuronium was infused at 5 microg x kg(-1) x min(-1) until the first response of each train-of-four had decreased by 70%. Arterial blood (for vecuronium analysis) was sampled at intervals until the first response recovered to at least 90% of its prevecuronium level. Vecuronium, 20 microg x kg(-1) x min(-1), was then infused for 10 min, and arterial blood was sampled at intervals for up to 7 h. Population-based nonlinear mixed-effects modeling was used to examine the effect of physical characteristics and core temperature on vecuronium pharmacokinetics and pharmacodynamics. Results Decreasing core temperature over 38.0-34.0 degrees C decreases the plasma clearance of vecuronium (11.3% per degrees C), decreases the rate constant for drug equilibration between plasma and effect site (0.023 min(-1) per degrees C), and increases the slope of the concentration-response relationship (0.43 per degrees C). Conclusions Our results show that reduced clearance and rate of effect site equilibration explain the increased duration of action of vecuronium with reducing core temperature. Tissue sensitivity to vecuronium is not influenced by core temperature.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Anesthesiology and Pain Medicine

Reference26 articles.

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