Clinical Significance of M1 Receptor Antagonists

Abstract

The M₁-selective antimuscarinic drugs pirenzepine and telenzepine moderately reduce gastric acid secretion without inhibiting smooth-muscle activity as much as nonselective antimuscarinics, e.g. atropine and 1-hyoscyamine. They hasten peptic ulcer healing and improve the symptoms of reflux oesophagitis. In combination with H₂ receptor antagonists they abolish gastric acid secretion almost completely and can therefore be used in high-risk peptic conditions. Long-term trials have to show whether they can form a medical alternative to parietal cell vagotomy. The effect of M₁-selective antimuscarinics on ‘nonulcer dyspepsia’ is equivocal, but they may possibly be useful in the treatment of spastic constipation.