Thiopental Does Not Produce Hyperalgesia: A Laboratory Study Using Two Human Experimental Pain Models

Author:

Arout Caroline A12ORCID,Petrakis Ismene L1,Ralevski Elizabeth1,Acampora Gregory3,Koretski Julia4,DeNegre Diana1,Newcomb Jenelle1,Perrino Albert C5

Affiliation:

1. Department of Psychiatry, Center for Translational Neuroscience of Alcoholism and VA Alcohol Research Center, Yale University School of Medicine, VA Connecticut Healthcare System, West Haven, Connecticut

2. Department of Psychiatry, Division on Substance Use Disorders, Columbia University Medical Center, New York State Psychiatric Institute, New York, New York

3. Department of Psychiatry, Massachusetts General Hospital, Harvard Center for Addiction Medicine, Boston, Massachusetts

4. University of Connecticut, School of Medicine, Farmington, Connecticut

5. Department of Anesthesiology, Yale School of Medicine, VA Connecticut Healthcare System, West Haven, Connecticut, USA

Abstract

Abstract Objective Past investigations assessing the effects of thiopental on pain are conflicting. Although several studies demonstrate hyperalgesia as a result of barbiturate administration, others show analgesia. Our objective was to assess the effects of an infusion of the GABAA agonist thiopental, compared with placebo, in healthy participants on two subjective experimental pain paradigms: noxious electrical stimulation and intradermal capsaicin. Methods For electrical stimulation, the milliamps required to achieve pain threshold and tolerance were recorded, and the percent change from baseline was determined for each infusion condition. In the intradermal capsaicin condition, the area of hyperalgesia was determined by von Frey technique pre- and postinfusion, and the percent change in the area of hyperalgesia was calculated. Results Though thiopental infusion resulted in an increase in the electrical stimulation current required to elicit pain threshold or reach pain tolerance when compared with baseline, this finding was not statistically significant. In the intradermal capsaicin condition, there was a statistically significant difference in overall pre- and postinfusion pain interpretation, as measured by the McGill Pain Questionnaire (P < 0.05), but there was no significant difference in area of hyperalgesia. Conclusions In this human study of thiopental’s effects on two experimental pain models, our results show that thiopental does not induce hyperalgesia.

Funder

Alcohol Beverage Medical Research Foundation, the Veterans Administration Merit

VA Alcohol Research Center

Center for the Translational Neuroscience of Alcoholism grant

C. A. Arout’s postdoctoral fellowship

NIH

Publisher

Oxford University Press (OUP)

Subject

Anesthesiology and Pain Medicine,Neurology (clinical),General Medicine

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