L‐694,247: a potent 5‐HT1D receptor agonist

Abstract

1 The 5-hydroxytryptamine (5-HT) receptor binding selectivity profile of a novel, potent 5-HT_1D receptor agonist, L-694,247 (2-[5-[3-(4-methylsulphonylamino)benzyl-1,2,4-oxadiazol-5-yl]-1H-indole-3-yl]ethylamine) was assessed and compared with that of the 5-HT₁-like receptor agonist, sumatriptan. 2 L-694,247 had an affinity (pIC₅₀) of 10.03 at the 5-HT_1D binding site and 9.08 at the 5-HT_1B binding site (sumatriptan: pIC₅₀ values 8.22 and 5.94 respectively). L-694,247 retained good selectivity with respect to the 5-HT_1A binding site (pIC₅₀ = 8.64), the 5-HT_1C binding site (6.42), the 5-HT₂ binding site (6.50) and the 5-HT_1E binding site (5.66). The pIC₅₀ values for sumatriptan at these radioligand binding sites were 6.14, 5.0, < 5.0 and 5.64 respectively. Both L-694,247 and sumatriptan were essentially inactive at the 5-HT₃ recognition site. 3 L-694,247, like sumatriptan, displayed a similar efficacy to 5-HT in inhibiting forskolin-stimulated adenylyl cyclase in guinea-pig substantia nigra although L-694,247 (pEC₅₀ = 9.1) was more potent than sumatriptan (6.2) in this 5-HT_1D receptor mediated functional response. L-694,247 (pEC₅₀ = 9.4) was also more potent than sumatriptan (6.5) in a second 5-HT_1D receptor mediated functional response, the inhibition of K⁺-evoked [³H]-5-HT release from guinea-pig frontal cortex slices. 4 The excellent agreement observed for L-694,247 between the 5-HT_1D radioligand binding affinity and the functional potency confirm that the two functional models (the inhibition of forskolin-stimulated adenylyl cyclase in guinea-pig substantia nigra and the inhibition of K⁺-evoked [³H]-5-HT release from guinea-pig frontal cortex) do indeed reflect 5-HT_1D-mediated events. 5 L-694,247 is a novel, highly potent 5-HT_1D/5-HT_1B receptor ligand which should prove useful for the exploration of the physiological role of these receptors in animals.