Table 1. In vitro binding affinities and in vivo pressor inhibition of orally administered ETAR and AT1R antagonists through development and optimization.
| Target receptor (s) | Antagonist name | ETAR Ki (nM) | AT1R Ki (nM) | ETBR Ki (nM) | AT2R Ki (nM) | Oral big ET-1 pressor (30 µM/kg) (AOC units)* | Oral Ang II pressor (30 µM/kg) (AOC units)* |
|---|---|---|---|---|---|---|---|
| ETAR | BMS-193884 | 1.4† | >10,000† | - | - | 10,100* | Inactive* |
| AT1R | Irbesartan | >10,000† | 1.1† | - | - | Inactive* | 11,940* |
| ETAR & AT1R | Unnamed biphenylsulfonamide | 39† | ND† | - | - | - | - |
| ETAR & AT1R | BMS-248360 | 1.9† | 10† | - | - | 7,900* | 6,000* |
| ETAR & AT1R | BMS-346567 (sparsentan) | 9.3* | 0.8* | >10,000* | >10,000* | 15,800* | 18,600* |
The chemical structures of the mono-selective antagonists BMS-193884 and irbesartan were merged to produce the first-generation dual ETAR/AT1R antagonist, an unnamed biphenylsulfonamide. Optimization regained the original target ETAR activity (BMS-248360). Further optimization retained dual specificity while improving bioavailability in dog and monkey and oral pressor inhibition in rat (BMS-346567/sparsentan, bioavailability data not shown).
Abbreviations: ‘-’ = not shown; AOC, area over curve, indicating potency and duration of action at equimolar doses; AT1R, AT1 receptor; ETAR, ET receptor type A; Ki, inhibitory constant; ND, not determined.
*
Murugesan 2005 [107].
†
Murugesan 2002 [2].