S(+)-ketamine Effect on Experimental Pain and Cardiac Output

Author:

Sigtermans Marnix1,Dahan Albert2,Mooren René3,Bauer Martin4,Kest Benjamin5,Sarton Elise4,Olofsen Erik6

Affiliation:

1. Doctoral Student.

2. Professor of Anesthesiology and Head of Research.

3. Laboratory Technician.

4. Staff Anesthesiologists.

5. Professor, Department of Psychology and Center for Developmental Neurosciences, The College of Staten Island, City University New York, New York, and Doctoral Program in Neuropsychology, Queens College, City University New York, Flushing, New York.

6. Research Associate, Department of Anesthesiology, Leiden University Medical Center, Leiden, The Netherlands.

Abstract

Background Low-dose ketamine behaves as an analgesic in the treatment of acute and chronic pain. To further understand ketamine's therapeutic profile, the authors performed a population pharmacokinetic-pharmacodynamic analysis of the S(+)-ketamine analgesic and nonanalgesic effects in healthy volunteers. Methods Ten men and ten women received a 2-h S(+)-ketamine infusion. The infusion was increased at 40 ng/ml per 15 min to reach a maximum of 320 ng/ml. The following measurements were made: arterial plasma S(+)-ketamine and S(+)-norketamine concentrations, heat pain intensity, electrical pain tolerance, drug high, and cardiac output. The data were modeled by using sigmoid Emax models of S(+)-ketamine concentration versus effect and S(+)-ketamine + S(+)-norketamine concentrations versus effect. Results Sex differences observed were restricted to pharmacokinetic model parameters, with a 20% greater elimination clearance of S(+)-ketamine and S(+)-norketamine in women resulting in higher drug plasma concentrations in men. S(+)-ketamine produced profound drug high and analgesia with six times greater potency in the heat pain than the electrical pain test. After ketamine-infusion, analgesia rapidly dissipated; in the heat pain test but not the electrical pain test, analgesia was followed by a period of hyperalgesia. Over the dose range tested, ketamine produced a 40-50% increase in cardiac output. A significant consistent contribution of S(+)-norketamine to overall effect was detected for none of the outcome parameters. Conclusions S(+)-ketamine displays clinically relevant sex differences in its pharmacokinetics. It is a potent analgesic at already low plasma concentrations, but it is associated with intense side effects.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Anesthesiology and Pain Medicine

Reference39 articles.

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