ObjectiveThe study was designed to investigate the effects of acetylcholine (ACh) on pulmonary circulation with special regard to mediators that could be involved in the mediation of ACh-induced effects. ACh has been reported to induce either vasodilation or vasoconstriction in the pulmonary circulation of different species.DesignProspective experimental study in rabbits.SettingExperimental laboratory in a university teaching hospital.SubjectsSixty-six adult rabbits of either sex.InterventionsThe experiments were performed on 66 isolated and ventilated rabbit lungs that were perfused with a cell- and plasma-free buffer solution. ACh was injected in various concentrations after pulmonary artery preconstriction and in untreated lungs.Measurements and Main ResultsPulmonary arterial pressure (PAP) and lung weight gain were monitored continuously. Perfusate samples were taken intermittently to determine endothelin-1 (ET-1), thromboxane A2(TXA2), and prostacyclin (PGI2) concentrations. ACh in final dosages from 10minus;5to 10minus;2M (n equals; 6 each) was injected into the pulmonary artery of lungs treated with U46619 to induce pulmonary arterial hypertension or was injected into untreated lungs. To analyze the potential mechanisms of action, ACh (10minus;5M) was administered in additional experiments after pretreatment with either ETAreceptor antagonist BQ123 (10minus;6M; n equals; 6) or the cyclooxygenase inhibitor diclofenac (10 mgr;g/mL; n equals; 6). In preconstricted pulmonary vessels, ACh (10minus;3and 10minus;2M) initially induced a PAP rise for 10 mins followed by a sustained decrease. In untreated lungs, ACh induced an immediate dose-dependent increase in PAP, requiring as long as 30 mins to return to predrug levels. Simultaneously, significantly elevated TXA2and PGI2levels were observed. Furthermore, ET-1 was detected in the perfusate, which was free from ET-1 before ACh administration. Pretreatment with BQ123 reduced substantially the ACh (10minus;5M)-induced PAP increase and the release of TXA2and PGI2. At 5 mins, the PAP maximum was reduced from 18.5 plusmn; 3.2 mm Hg to 9.9 plusmn; 0.65 mm Hg by BQ123 pretreatment (p .01). An inhibition of PAP increase was also observed after diclofenac pretreatment (11.6 plusmn; 0.4 mm Hg at 5 mins;p .05). Inhibitory effects at 5 mins were significantly more pronounced in the BQ123 group compared with the diclofenac group.ConclusionsThe effects of ACh on the pulmonary circulation of isolated rabbit lungs depend on ACh concentration and the basal tone of the arterial vasculature. In lungs with a normal pulmonary vascular resistance, ACh administration causes vasoconstriction via the release of ET-1 and TXA2, whereas vasodilation is induced in preconstricted pulmonary vessels.
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