摘要:The pharmacological properties of SWR-0315NA, ( E , Z )-[4[[1-[2-[(3-phenoxy-2-hydroxy propyl)]amino]ethyl]-1-propenyl]phenoxy]acetic acid sodium, were compared with those of (−)-isoproterenol. In the radioligand binding studies of [125I]iodocyanopindolol with COS-7 cell membranes that transiently expressed human β-adrenoceptor (β-AR) subtypes, SWR-0315NA exhibited 1-fold and 2-fold greater binding affinities for β3-AR than those for β1- and β2-ARs, respectively. The maximal stimulatory effects of SWR-0315NA on cAMP accumulation in CHO cells expressing all the β-AR subtypes were 79%, 3% and 93% for β1-, β2- and β3-ARs of those produced by (−)-isoproterenol, respectively. SWR-0315NA has 26.3-fold and more than 630-fold greater selectivity for β3-AR than those for β1- and β2-ARs in potency, respectively. These results indicate that although SWR-0315NA has lower binding selectivity towards β-AR subtypes, it is a selective agonist with high intrinsic activity for β3-AR as compared with (−)-isoproterenol.
