Vendor-derived differences in injury-induced pain phenotype and pharmacology of Sprague-Dawley rats: Does it matter?

P J Kristensen; A M Heegaard; S Hestehave; R D Jeggo; O J Bjerrum; G Munro

doi:10.1002/ejp.973

Vendor-derived differences in injury-induced pain phenotype and pharmacology of Sprague-Dawley rats: Does it matter?

Eur J Pain. 2017 Apr;21(4):692-704. doi: 10.1002/ejp.973. Epub 2016 Nov 2.

Authors

P J Kristensen^{1

2}, A M Heegaard¹, S Hestehave^{2

3}, R D Jeggo², O J Bjerrum¹, G Munro²

Affiliations

¹ Department of Drug Design and Pharmacology, Faculty of Health and Medical Sciences, University of Copenhagen, Denmark.
² Department of In Vivo Neurodegeneration, H. Lundbeck A/S, Valby, Denmark.
³ Department of Experimental Medicine, Faculty of Health and Medical Sciences, University of Copenhagen, Denmark.

PMID: 27805755
DOI: 10.1002/ejp.973

Abstract

Background: Outbred Sprague-Dawley (SD) rats are a commonly used strain in preclinical pain research. Here, we established empirically how SD rats obtained from different vendors might vary in sensitivity to injury and pharmacotherapy.

Methods: Chronic Constriction Injury (CCI) or complete Freund's adjuvant (CFA) hindpaw inflammation was induced in male SD rats sourced from three to four different vendors, respectively. Neuropathic hypersensitivity was evaluated over 58 days using von Frey filaments, pinprick stimulation and the hot plate test. Pharmacological sensitivity was evaluated by treatment with gabapentin (100 mg/kg, p.o.) or morphine (3 mg/kg, s.c.). CFA-induced hyperalgesia and sensitivity to morphine (0.3-6 mg/kg, s.c.) was measured using a digital Randall-Selitto device. In addition, paw weight gain was used as an index of peripheral oedema.

Results: Significant differences between the vendor-supplied SD rats in relation to onset, magnitude and resolution of hypersensitivity after CCI were observed. Although all sub-strains eventually developed a robust and reversible neuropathic hypersensitivity to mechanical stimulation, the thermal hypersensitivity varied. Whereas pharmacological response to gabapentin varied enormously, the response to morphine was both robust and much more consistent between sub-strains. Despite a similar degree of CFA-induced hypersensitivity, the paw oedema level differed between sub-strains. Here, morphine dose-dependently alleviated the CFA-induced hypersensitivity, with only a subtle difference in sensitivity between sub-strains observed.

Conclusions: Our data reveal that the source of vendor used to obtain SD rats may be one key factor responsible for 'between laboratory variation' in reproducing sensitivity to some drugs targeting various pathophysiological mechanisms in specific animal pain models.

Significance: The choice of vendor used to source the same strain of rat for use in preclinical pain research can profoundly affect the level of nociceptive hypersensitivity and response to reference analgesics in neuropathic versus inflammatory models.

MeSH terms

Amines / therapeutic use*
Analgesics / therapeutic use*
Animals
Cyclohexanecarboxylic Acids / therapeutic use*
Freund's Adjuvant
Gabapentin
Hyperalgesia / drug therapy
Hyperalgesia / etiology
Hyperalgesia / physiopathology*
Inflammation / drug therapy
Male
Morphine / therapeutic use*
Neuralgia / drug therapy
Neuralgia / etiology
Neuralgia / physiopathology*
Pain Measurement
Phenotype
Rats
Rats, Sprague-Dawley
Species Specificity
Treatment Outcome
gamma-Aminobutyric Acid / therapeutic use*

Substances

Amines
Analgesics
Cyclohexanecarboxylic Acids
gamma-Aminobutyric Acid
Gabapentin
Morphine
Freund's Adjuvant