Selective and non-selective et antagonists reveal an ETA/ETB receptor mediated ET-1-induced antinociceptive effect in PAG area of mice |
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Affiliation: | Professor of Global Surgery/Urology, Adjunct Assoc. Professor, Public Health, University of Utah School of Medicine, Center for Global Surgery, Salt Lake City, UT |
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Abstract: | The injection of endothelin-1 (ET-1) (2 pmol) into the dorsolateral periaqueductal gray area (PAG) of mice produces antinociceptive effect as underscored by increases in the latency time for the reaction to a hot plate. Pretreatment of the PAG area with bosentan (10 nmol) (a mixed ETA/ETB receptor antagonist), FR 139317 (5 nmol) (ETA receptor selective antagonist) or BQ-788 (5 nmol) (ETB receptor selective antagonist) greatly reduced the antinociceptive effect induced by ET-1. Therefore, ET-1 induces antinociceptive effects via both ETA/ETB receptors. In addition, since ET-antagonists lowered per se the control reaction time of the mice when administered alone to the PAG area, we would suggest that endogenous ET-1 acting within the PAG area contributes to the suppression of pain. |
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