The erythromycin derivative EM-523 is a potent motilin agonist in man and in rabbit

Abstract

Erythromycin may stimulate gastrointestinal motor activity via its effect upon motilin receptors. We have studied the ability of the derivative EM-523 [de(N-methyl)-N-ethyl-8,9-anhydroerythromycin A 6,9-hemiacetal] to induce contractions in duodenal smooth muscle strips and to displace labeled motilin bound to antral smooth muscle, in man and in rabbit. In both species EM-523 approached the potency of motilin for inducing contractions. Thus pED 50 values were 7.84±0.11 and 8.69±0.12 for motilin in, respectively, man and rabbit, against 6.08±0.13 and 8.19±0.10 for EM-523. In rabbit the efficacy of both compounds decreased in parallel aborally, the responses to EM-523 could not be blocked by atropine (10 −7 M) or TTX (10 −7 M), and both compounds were unable to further enhance the maximum effect to the other compound. In binding studies the order of potency was the same as in the contraction studies. The pIC 50 values were: motilin ( 8.84±0.31, 9.17±0.20) > EM-523 ( 7.89±0.1, 8.40±0.10). A Schild plot revealed that EM-523 was a competitive inhibitor of motilin receptor binding in man and in rabbit. We conclude that EM-523 is a potent motilin agonist.