GABA B receptor-mediated mechanisms in human intestine in vitro

Abstract

The spontaneous motility of longitudinal muscle of human jejunum was recorded and the effect of γ-aminobutyric acid-ergic (GABAergic) drugs was tested. GABA and (−)-baclofen (10 −6−10 −4 M) dose dependently reduced the amplitude and frequency of the spontaneous contractions; muscimol and 3-aminopropanesulfonic acid (3 × 10 −5 M) were ineffective. The effect of 3 × 10 −5 M GABA was reduced by 3 × 10 −3 M 5-aminovaleric acid but not by 3 × 10 −5 M picrotoxin. The dose-response curve for GABA was shifted to the right by 3 × 10 −3 M 3-aminopropanesulfonic acid. Tetrodotoxin 3 × 10 −7 M prevented the GABAergic action, whereas various receptor antagonists tested did not affect it. GABAergic drugs did not influence the spontaneous motility of either circular or longitudinal muscles of human colon. It is suggested that GABA B receptor activation induces the inhibition of human jejunum longitudinal muscle motility by a neurogenic mechanism. The possible involvement of postganglionic cholinergic neurons is to be evaluated by other techniques.