Oshiro Y, Sato S, Kurahashi N, Tanaka T, Kikuchi T, Tottori K, Uwahodo Y, Nishi T
Third Institute of New Drug Research, Otsuka Pharmaceutical Company Ltd., Tokushima, Japan.
J Med Chem. 1998 Feb 26;41(5):658-67. doi: 10.1021/jm940608g.
To develop a novel antipsychotic agent which is an agonist of dopamine (DA) autoreceptors and an antagonist of postsynaptic DA receptors, a series of 7-[4-[4-(substituted phenyl)-1-piperazinyl]butoxy]-3,4-dihydro-2 (1H)-quinolinones was synthesized and their dual activities were examined. The postsynaptic DA receptor antagonistic activities of the compounds were evaluated by their ability to inhibit stereotypy induced by apomorphine in mice, and the autoreceptor agonist activities were determined by their effects on the gamma-butyrolactone (GBL)-induced increase in L-dihydroxyphenylalanine (DOPA) synthesis in the mouse brain. Many compounds inhibited the stereotypic behavior, and several compounds reversed the GBL-induced increase in the DOPA synthesis. Among them, 7-[4-[4-(2,3-dichlorophenyl)-1-piperazinyl]-butoxy]-3,4-dihydro-2 (1H)-quinolinone (28, aripiprazole, OPC-14597) was found to have these two activities. This compound reversed the GBL-induced DOPA synthesis (ED50 values of 5.1 mumol/kg p.o.) and inhibited the APO induced stereotypy (ED50 values of 0.6 mumol/kg p.o.). Compound 28 induced catalepsy at 10 times higher dose than that required for the antagonism of APO-induced stereotypy (ED50 value of 7.8 mumol/kg p.o.).
为了开发一种新型抗精神病药物,它是多巴胺(DA)自身受体的激动剂和突触后DA受体的拮抗剂,合成了一系列7-[4-[4-(取代苯基)-1-哌嗪基]丁氧基]-3,4-二氢-2(1H)-喹啉酮,并检测了它们的双重活性。通过化合物抑制阿扑吗啡诱导的小鼠刻板行为的能力来评估其突触后DA受体拮抗活性,通过它们对γ-丁内酯(GBL)诱导的小鼠脑内L-二羟基苯丙氨酸(DOPA)合成增加的影响来确定自身受体激动剂活性。许多化合物抑制了刻板行为,几种化合物逆转了GBL诱导的DOPA合成增加。其中,7-[4-[4-(2,3-二氯苯基)-1-哌嗪基]丁氧基]-3,4-二氢-2(1H)-喹啉酮(28,阿立哌唑,OPC-14597)被发现具有这两种活性。该化合物逆转了GBL诱导的DOPA合成(口服给药的ED50值为5.1μmol/kg)并抑制了阿扑吗啡诱导的刻板行为(口服给药的ED50值为0.6μmol/kg)。化合物28诱导僵住症的剂量比拮抗阿扑吗啡诱导的刻板行为所需剂量高10倍(口服给药的ED50值为7.8μmol/kg)。
