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Canadian Journal of Anesthesia/Journal canadien d'anesthésie

Erschienen in:

01.08.2013 | Reports of Original Investigations

Evaluation of a novel mouse model of intracisternal strychnine-induced trigeminal allodynia

verfasst von: Il-Ok Lee, PhD, Ryan A. Whitehead, BSc, Craig R. Ries, MD, PhD, Stephan K. W. Schwarz, MD, PhD, Ernest Puil, PhD, Bernard A. MacLeod, MD

Erschienen in: Canadian Journal of Anesthesia/Journal canadien d'anesthésie | Ausgabe 8/2013

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Abstract

Purpose

Intractable neuropathic dynamic allodynia remains one of the major symptoms of human trigeminal neuropathy and is commonly accepted to be the most excruciatingly painful condition known to humankind. At present, a validated animal model of this disorder is necessary for efficient and effective development of novel drug treatments. Intracisternal strychnine in rats has been shown to result in localized trigeminal dynamic allodynia, thus representing a possible model of trigeminal neuralgia. The purpose of this study was to validate a mouse model of trigeminal glycinergic inhibitory dysfunction using established positive (carbamazepine epoxide) and negative (morphine) controls.

Methods

The actions of conventional first-line treatment (carbamazepine epoxide [CBZe]) and clinically ineffective morphine were tested for trigeminal dynamic mechanical allodynia produced by intracisternal strychnine. In mice under halothane anesthesia, we injected either strychnine (0.3 μg), strychnine with CBZe (4 ng), or artificial cerebrospinal fluid (aCSF) intracisternally (i.c.). In a separate set of experiments, subcutaneous morphine (3 mg·kg⁻¹ sc) was injected with intracisternal strychnine. Dynamic mechanical allodynia was induced by stroking the fur with polyethylene (PE-10) tubing. The response of each mouse was rated to determine its allodynia score, and scores of each group were compared. In addition, in a separate dichotomous disequilibrium study, pairs of mice were injected with strychnine/saline, strychnine/strychnine-CBZe, or strychnine/strychnine-morphine. A blinded observer recorded which mouse of each pair had the greater global pain behaviour.

Results

Strychnine (i.c.) produced higher quantitative allodynia scores in the trigeminal distribution (mean 81.5%; 95% confidence interval [CI] 76.4 to 86.6) vs the aCSF group (mean 11.3%; 95% CI 8.1 to 14.4) (P < 0.0001). Carbamazepine epoxide (i.c.) completely abolished allodynia when co-injected with strychnine (mean 83.2%; 95% CI 78.1 to 88.4) vs strychnine alone (mean 3.2%; 95% CI −0.9 to 7.2) (P < 0.0001). Morphine co-injected with strychnine did not result in reduced allodynia (mean 65.7%; 95% CI 42.0 to 89.4) compared with strychnine alone (mean 87.6%; 95% CI 77.6 to 97.6) (P = 0.16). In a further global allodynia assessment, strychnine (i.c.) produced greater allodynia than both aCSF and strychnine administered with CBZe (P = 0.03). Morphine (ip) administered with strychnine did not result in reduced global allodynia compared with strychnine administered alone (P = 1.0).

Conclusion

In this study, we have developed and validated a novel murine model of trigeminal dynamic allodynia induced by intracisternal strychnine. The use of mice to study trigeminal allodynia has many benefits, including access to a vast repository of transgenic mouse variants, ease of handling, low cost, and minimal variance of results. The present model may have utility in screening drug treatments for dynamic mechanical allodynia resulting from trigeminal neuropathies.

Costigan M, Scholz J, Woolf CJ. Neuropathic pain: a maladaptive response of the nervous system to damage. Ann Rev Neurosci 2009; 32: 1-32.PubMedCrossRef

Okeson JP. Bell’s Orofacial Pains: The Clinical Management of Orofacial Pain. 6th ed. Chicago: Quintessence Publishing Co. Ltd; 2005.

Kitt CA, Gruber K, Davis M, Woolf CJ, Levine JD. Trigeminal neuralgia: opportunities for research and treatment. Pain 2000; 85: 3-7.PubMedCrossRef

Miraucourt LS, Moisset X, Dallel R, Voisin DL. Glycine inhibitory dysfunction induces a selectively dynamic, morphine-resistant, and neurokinin 1 receptor-independent mechanical allodynia. J Neurosci 2009; 29: 2519-27.PubMedCrossRef

Miraucourt LS, Dallel R, Voisin DL. Glycine inhibitory dysfunction turns touch into pain through PKCgamma interneurons. PLoS One 2007; 2: e1116.PubMedCrossRef

Dickenson AH, Kieffer B. Opiates: basic mechanisms. In: McMahon SB, Koltzenburg M, editors. Wall and Melzack’s Textbook of Pain. 5th ed. Philadelphia: Churchill Livingstone; 2006. p. 427-42.CrossRef

van Kleef M, van Genderen WE, Narouze S, et al. 1. Trigeminal neuralgia. Pain Pract 2009; 9: 252-9.PubMedCrossRef

Lee IO, Son JK, Lim ES, Kim YS. Pharmacology of intracisternal or intrathecal glycine, muscimol, and baclofen in strychnine-induced thermal hyperalgesia of mice. J Korean Med Sci 2011; 26: 1371-7.PubMedCrossRef

Tomson T, Bertilsson L. Potent therapeutic effect of carbamazepine-10,11-epoxide in trigeminal neuralgia. Arch Neurol 1984; 41: 598-601.PubMedCrossRef

10.

Vos BP, Strassman AM, Maciewicz RJ. Behavioral evidence of trigeminal neuropathic pain following chronic constriction injury to the rat’s infraorbital nerve. J Neurosci 1994; 14: 2708-23.PubMed

11.

Juni A, Klein G, Kest B. Morphine hyperalgesia in mice is unrelated to opioid activity, analgesia, or tolerance: evidence for multiple diverse hyperalgesic systems. Brain Res 2006; 1070: 35-44.PubMedCrossRef

12.

Mansikka H, Zhao C, Sheth RN, Sora L, Uhl G, Raja SN. Nerve injury induces a tonic bilateral mu-opioid receptor-mediated inhibitory effect on mechanical allodynia in mice. Anesthesiology 2004; 100: 912-21.PubMedCrossRef

13.

Zarbin MA, Wamsley JK, Kuhar MJ. Glycine receptor: light microscopic autoradiographic localization with [3H] strychnine. J Neurosci 1981; 1: 532-47.PubMed

14.

Betz H, Laube B. Glycine receptors: recent insights into their structural organization and functional diversity. J Neurochem 2006; 97: 1600-10.PubMedCrossRef

15.

Ghavanini AA, Mathers DA, Puil E. Glycinergic inhibition in thalamus revealed by synaptic receptor blockade. Neuropharmacology 2005; 49: 338-49.PubMedCrossRef

16.

Holtman JR Jr, Buller AL, Hamosh P, Da Silva AM, Gillis RA. Respiratory depression produced by glycine injected into the cisterna magna of cats. Neuropharmacology 1982; 11: 1223-5.CrossRef

17.

Davidoff RA, Aprison MH, Werman R. The effects of strychnine on the inhibition of interneurons by glycine and gamma-aminobutyric acid. Int J Neuropharmacol 1969; 8: 191-4.PubMedCrossRef

18.

MacLeod BA, Wang JT, Chung CC, Ries CR, Schwarz SK, Puil E. Analgesic properties of the novel amino acid, isovaline. Anesth Analg 2012; 110: 1206-14.CrossRef

19.

Whitehead RA, Puil E, Ries CR, et al. GABA(B) receptor-mediated selective peripheral analgesia by the non-proteinogenic amino acid, isovaline. Neuroscience 2012; 213: 154-60.PubMedCrossRef

20.

Terrence CF, Sax M, Fromm GH, Chang CH, Yoo CS. Effect of baclofen enantiomorphs on the spinal trigeminal nucleus and steric similarities of carbamazepine. Pharmacology 1983; 27: 85-94.PubMedCrossRef

21.

Fromm GH, Terrence CF. Comparison of L-baclofen and racemic baclofen in trigeminal neuralgia. Neurology 1987; 37: 1725-8.PubMedCrossRef

Titel: Evaluation of a novel mouse model of intracisternal strychnine-induced trigeminal allodynia
verfasst von: Il-Ok Lee, PhD
Ryan A. Whitehead, BSc
Craig R. Ries, MD, PhD
Stephan K. W. Schwarz, MD, PhD
Ernest Puil, PhD
Bernard A. MacLeod, MD
Publikationsdatum: 01.08.2013
Verlag: Springer US
Erschienen in: Canadian Journal of Anesthesia/Journal canadien d'anesthésie / Ausgabe 8/2013
Print ISSN: 0832-610X
Elektronische ISSN: 1496-8975
DOI: https://doi.org/10.1007/s12630-013-9975-x

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Evaluation of a novel mouse model of intracisternal strychnine-induced trigeminal allodynia