Effect of genetic deletion and pharmacological antagonism of P2X7 receptors in a mouse animal model of migraine: Doc 610

Purine receptors participate in peripheral and central sensitization and are associated with migraine headache. We investigated the role of P2X7 receptor (P2X7) in a nitroglycerin (NTG)-induced mouse model of migraine. Intraperitoneal NTG injection (15 mg/kg) triggered thermal hyperalgesia in the hi...

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Bibliographic Details
Published in:Journal of headache and pain 2014-05, Vol.15, p.1
Main Authors: Gölöncsér, Flóra, Sperlágh, Beáta
Format: Article
Language:English
Subjects:
Antagonist drugs
Genetics
Migraine
Pathogenesis
Rodents
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Summary:Purine receptors participate in peripheral and central sensitization and are associated with migraine headache. We investigated the role of P2X7 receptor (P2X7) in a nitroglycerin (NTG)-induced mouse model of migraine. Intraperitoneal NTG injection (15 mg/kg) triggered thermal hyperalgesia in the hindpaws of wild-type C57BL/6J mice, followed by the induction of c-fos in upper cervical spinal cord and trigeminal nucleus caudalis. The effect of genetic deletion of P2X7 and the selective P2X7 antagonist Brilliant Blue G (BBG) were examined on hyperalgesia and c-fos induction. NTG decreased the paw withdrawal threshold in both wild-type and P2X7 knockout mice. Nevertheless, subacute BBG treatment (50 mg/kg/day i.p.) completely prevented the effect of NTG in wild-type, but not in knockout mice. Whereas P2X7 deficiency differentially affected the expression of c-fos, the average number of fos-immuno-reactive neurons in trigeminal nucleus caudalis, but not in upper cervical spinal cord was lower in BBG-treated wild-type mice after NTG treatment. Our results show that P2X7 receptors might participate in the pathogenesis of migraine, although upregulation of other P2X receptors probably compensate for the loss of its action in knockout mice. The data also suggest the therapeutic potential of P2X7 antagonists for the treatment of migraine.[PUBLICATION ABSTRACT]
ISSN:1129-2369
1129-2377
DOI:10.1186/1129-2377-15-24