Antinociception by Spinal and Systemic Oxycodone: Why Does the Route Make a Difference?-Reference-Cited by-同舟云学术

Antinociception by Spinal and Systemic Oxycodone: Why Does the Route Make a Difference?

Published:2006-10-01 Issue:4 Volume:105 Page:801-812
ISSN:0003-3022
Container-title:Anesthesiology
language:en
Short-container-title:

Author:

Lemberg Kim K.¹,Kontinen Vesa K.²,Siiskonen Antti O.¹,Viljakka Kaarin M.¹,Yli-Kauhaluoma Jari T.³,Korpi Esa R.⁴,Kalso Eija A.⁵

Affiliation:

1. Ph.D. Student.

2. Senior Researcher.

3. Professor, Faculty of Pharmacy, Division of Pharmaceutical Chemistry, University of Helsinki.

4. Professor, Department of Pharmacology, Institute of Biomedicine.

5. Professor, Department of Pharmacology, Institute of Biomedicine, University of Helsinki, and Department of Anesthesia and Intensive Care Medicine, Helsinki University Central Hospital.

Abstract

Background The pharmacology of oxycodone is poorly understood despite its growing clinical use. The discrepancy between its good clinical effectiveness after systemic administration and the loss of potency after spinal administration led the authors to study the pharmacodynamic effects of oxycodone and its metabolites using in vivo and in vitro models in rats. Methods Male Sprague-Dawley rats were used in hot-plate, tail-flick, and paw-pressure tests to study the antinociceptive properties of morphine, oxycodone, and its metabolites oxymorphone and noroxycodone. Mu-opioid receptor agonist-stimulated GTPgamma[S] autoradiography was used to study G-protein activation induced by morphine, oxycodone, and oxymorphone in the rat brain and spinal cord. Spontaneous locomotor activity was measured to assess possible sedation or motor dysfunction. Naloxone and the selective kappa-opioid receptor antagonist nor-binaltorphimine were used to study the opioid receptor selectivity of the drugs. Results Oxycodone showed lower efficacy and potency to stimulate GTPgamma[S] binding in the spinal cord and periaqueductal gray compared with morphine and oxymorphone. This could relate to the fact that oxycodone produced only weak naloxone-reversible antinociception after intrathecal administration. It also suggests that the metabolites may have a role in oxycodone-induced analgesia in rats. Intrathecal oxymorphone produced strong long-lasting antinociception, whereas noroxycodone produced antinociception with very high doses only. Subcutaneous administration of oxycodone and oxymorphone produced thermal and mechanical antinociception that was reversed by naloxone but not by nor-binaltorphimine. Oxymorphone was more potent than oxycodone, particularly in the hot-plate and paw-pressure tests. Conclusions The low intrathecal potency of oxycodone in rats seems be related to its low efficacy and potency to stimulate mu-opioid receptor activation in the spinal cord.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Anesthesiology and Pain Medicine

Link

http://pubs.asahq.org/anesthesiology/article-pdf/105/4/801/360752/0000542-200610000-00027.pdf

Reference47 articles.

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