Synthesis of Dihydrofuroaporphine Derivatives: Identification of a Potent and Selective Serotonin 5-HT_1A Receptor Agonist

Abstract: A series of new aporphine analogues were synthesized and pharmacologically evaluated. 11-Allyloxy-(17), 11-propargyloxy-(20), and dihydrofuro-(19) aporphines displayed the highest affinity at the 5-HT(1A) receptor with K(i) values of 12.0, 14.0, and 6.7 nM, respectively. The high binding potential of the diastereomeric mixture of aporphine 19 was found residing in the cis-diastereomer (cis-19). [(35)S]GTP gamma S function assays on 5-HT(1A) receptor indicated that aporphines 17 and 20 were partial agonists, wh… Show more

“…Therefore, to quickly identify new compounds for further study, all compounds in current report were prepared and evaluated as racemates. As shown in Scheme 1, by following a literature procedure [12,13,22,23], 7-and 8-methoxy-N-methyl-1-benzazepines 7 and 8 were prepared from corresponding 3-or 4-methoxyphenyl ethanamine and 2-phenyloxirane in three steps [18,19]. Removal [23] of the Omethyl group by refluxing in 48% HBr aqueous solution led to monohydroxyl benzazepines 9 and 10 in 90% yield.…”

“…As shown in Scheme 1, by following a literature procedure [12,13,22,23], 7-and 8-methoxy-N-methyl-1-benzazepines 7 and 8 were prepared from corresponding 3-or 4-methoxyphenyl ethanamine and 2-phenyloxirane in three steps [18,19]. Removal [23] of the Omethyl group by refluxing in 48% HBr aqueous solution led to monohydroxyl benzazepines 9 and 10 in 90% yield. Nitration of 8-hydroxy-N-methyl-1-phenylbenzazepine 10 with fuming HNO 3 and HOAc provided compounds 11 and 11 0 in 96% overall yield, with nearly no regioselectivity (1.1/1).…”

“…Acylation of amine 12 led to benzazepine 14 in 41% yield, and diethylamino-substituted benzazepine 15 was prepared in 81% yield by treating 12 with acetaldehyde and NaBH(OAc) 3 . Meanwhile, treatment [24] of 12 with 2,5-dimethoxy- Aryl methanol 18 was prepared [23] by treating phenol 9 with formaldehyde and anhydrous MgCl 2 in refluxing THF, followed by reduction with NaBH 4 in 45% overall yield (Scheme 2). Meanwhile, the benzaldehyde intermediate 17 was reacted with hydroxylamine hydrochloride followed by reduction with LiAlH 4 to afford phenylmethyl amine 19 in 58% overall yield [24].…”

“…Bromination of 8-methoxy-3-H-benzazepine 8 0 followed by N-methylation provided bromide 20 in 40% yield, which was then subjected to palladium-catalyzed Suzuki coupling with arylboronic acids followed by O-demethylation [22] with BBr 3 at À78 C to deliver target compounds 21aee in 27e73% overall yields. Meanwhile, triflation of 7-and 8-hydroxylbenzazepines 9 and 10 with Tf 2 O and Et 3 N, followed by Pd(OAc) 2 -catalyzed CeN bond formation [23] and subsequent hydrolysis provided 7-and 8-aminobenzazepines 22 and 23 in 82% overall yields. N-Methylation was completed by treating amine 23 with ethyl formate followed by LiAlH 4 giving benzazepine 24 in 48% overall yield.…”

Structural manipulation on the catecholic fragment of dopamine D1 receptor agonist 1-phenyl-N-methyl-benzazepines

“…Therefore, to quickly identify new compounds for further study, all compounds in current report were prepared and evaluated as racemates. As shown in Scheme 1, by following a literature procedure [12,13,22,23], 7-and 8-methoxy-N-methyl-1-benzazepines 7 and 8 were prepared from corresponding 3-or 4-methoxyphenyl ethanamine and 2-phenyloxirane in three steps [18,19]. Removal [23] of the Omethyl group by refluxing in 48% HBr aqueous solution led to monohydroxyl benzazepines 9 and 10 in 90% yield.…”

“…As shown in Scheme 1, by following a literature procedure [12,13,22,23], 7-and 8-methoxy-N-methyl-1-benzazepines 7 and 8 were prepared from corresponding 3-or 4-methoxyphenyl ethanamine and 2-phenyloxirane in three steps [18,19]. Removal [23] of the Omethyl group by refluxing in 48% HBr aqueous solution led to monohydroxyl benzazepines 9 and 10 in 90% yield. Nitration of 8-hydroxy-N-methyl-1-phenylbenzazepine 10 with fuming HNO 3 and HOAc provided compounds 11 and 11 0 in 96% overall yield, with nearly no regioselectivity (1.1/1).…”

“…Acylation of amine 12 led to benzazepine 14 in 41% yield, and diethylamino-substituted benzazepine 15 was prepared in 81% yield by treating 12 with acetaldehyde and NaBH(OAc) 3 . Meanwhile, treatment [24] of 12 with 2,5-dimethoxy- Aryl methanol 18 was prepared [23] by treating phenol 9 with formaldehyde and anhydrous MgCl 2 in refluxing THF, followed by reduction with NaBH 4 in 45% overall yield (Scheme 2). Meanwhile, the benzaldehyde intermediate 17 was reacted with hydroxylamine hydrochloride followed by reduction with LiAlH 4 to afford phenylmethyl amine 19 in 58% overall yield [24].…”

“…Bromination of 8-methoxy-3-H-benzazepine 8 0 followed by N-methylation provided bromide 20 in 40% yield, which was then subjected to palladium-catalyzed Suzuki coupling with arylboronic acids followed by O-demethylation [22] with BBr 3 at À78 C to deliver target compounds 21aee in 27e73% overall yields. Meanwhile, triflation of 7-and 8-hydroxylbenzazepines 9 and 10 with Tf 2 O and Et 3 N, followed by Pd(OAc) 2 -catalyzed CeN bond formation [23] and subsequent hydrolysis provided 7-and 8-aminobenzazepines 22 and 23 in 82% overall yields. N-Methylation was completed by treating amine 23 with ethyl formate followed by LiAlH 4 giving benzazepine 24 in 48% overall yield.…”

Structural manipulation on the catecholic fragment of dopamine D1 receptor agonist 1-phenyl-N-methyl-benzazepines

“…[ 35 S]GTPγS binding assays 26 were employed to determine the agonistic or antagonistic activities of compounds with K i values less than 130 nM (5b, 5c, 5d, 5i, 5k, 5o, 5m 5n), in which olanzapine was used as reference compound. The potent antagonist olanzapine of 5-HT 2A was also used as reference compound.…”

Discovery of novel potent and selective ligands for 5-HT2A receptor with quinazoline scaffold

Mechanistic Studies on the Stereoselectivity of the Serotonin 5‐HT_1A Receptor