Effect of M₂ and M₃ Muscarinic Receptors on Airway Responsiveness to Carbachol in Bronchial-Hypersensitive (BHS) and Bronchial-Hyposensitive (BHR) Guinea Pigs

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The expression balance of M₂ and M₃ muscarinic receptor subtypes on the pathogenesis of airway hyperresponsiveness was investigated by using two congenitally related strains of guinea pigs, bronchial-hypersensitive (BHS) and bronchial-hyposensitive (BHR). CCh-induced airway responses in vivo and in vitro were investigated by comparing the effects of muscarinic receptor subtype antagonists, and the relative amounts of M₂ and M₃ muscarinic receptor mRNA in tracheal smooth muscle and lung tissue were investigated. After treatment with muscarinic receptor subtype antagonists, the ventilatory mechanics (V_T, R_aw, and C_dyn) of response to CCh aerosol inhalation were measured by the bodyplethysmograph method. The effects of these antagonists on CCh-induced tracheal smooth muscle contraction were also investigated. The effects of M₂ muscarinic receptor blockade were less but the effects of M₃ muscarinic receptors blockade on the airway contractile responses were greater in BHS than in BHR. In M₃ muscarinic receptor blockades, CCh-induced tracheal contractions in BHS were significantly greater than those in BHR. In tracheal smooth muscle from BHS, the relative amount of M₂ muscarinic receptors mRNA was less but that of M₃ muscarinic receptor mRNA was more than those in BHR. These results suggest that the high ACh level as a consequence of dysfunction of M₂ muscarinic autoreceptors and the excessive effect of M₃ muscarinic receptors on the airway smooth muscle may play an important role in the pathogenesis of airway hyperresponsiveness.