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新型抗精神病药物OPC-4392的1期研究。

Phase 1 study of a new antipsychotic drug, OPC-4392.

作者信息

Murasaki M, Miura S, Ishigooka J, Ishii Y, Takahashi A, Fukuyama Y

机构信息

Department of Psychiatry, Kitasato University School of Medicine, Sagamihara, Japan.

出版信息

Prog Neuropsychopharmacol Biol Psychiatry. 1988;12(5):793-802. doi: 10.1016/0278-5846(88)90024-3.

Abstract
  1. A phase I study of OPC-4392 (OPC), a quinolinone derivative recently developed in Japan and recognized to have an agonistic effect on dopamine autoreceptors, was performed in 7 male healthy volunteers in comparison with chlorpromazine (CPZ). 2. Clinical pharmacology The main clinical symptoms of OPC were sleepiness, weakness, fatigability, heavy headedness, disturbance of concentration, nausea, etc. The severity of these symptoms increased dose-dependently, and the upper limit dosage of OPC was considered to be 5 mg for the healthy volunteers. 3. Endocrinological research The serum prolactin level decreased dose-dependently in the OPC group, whereas it rose in the CPZ group. A significant negative correlation was recognized between the OPC-plasma level and serum prolactin level as well. 4. Psychological tests In the Kraepelin test, a decrease in the average work quantity was observed in both groups, but it was less in the OPC group. 5. Pharmacokinetic study From the pharmacokinetic parameters measured, two features were recognized: one was the slowness of Tmax (4-6 hours) and the other was the length of its biological half-life (56-88 hours). It was estimated that the plasma level of OPC-4392 would take 2 weeks to reach a steady state.
摘要
  1. 对OPC-4392(OPC)进行了一项I期研究,该喹啉酮衍生物最近在日本研发,被认为对多巴胺自身受体有激动作用,研究选取了7名男性健康志愿者,并与氯丙嗪(CPZ)进行比较。2. 临床药理学OPC的主要临床症状为嗜睡、虚弱、易疲劳、头晕、注意力不集中、恶心等。这些症状的严重程度呈剂量依赖性增加,健康志愿者的OPC上限剂量被认为是5毫克。3. 内分泌学研究OPC组血清催乳素水平呈剂量依赖性下降,而CPZ组则上升。OPC血浆水平与血清催乳素水平之间也存在显著的负相关。4. 心理测试在克雷佩林测试中,两组的平均工作量均有所下降,但OPC组下降较少。5. 药代动力学研究从所测的药代动力学参数来看,有两个特点:一是达峰时间(Tmax)较慢(4至6小时),另一个是其生物半衰期较长(56至88小时)。据估计,OPC-4392的血浆水平需要2周才能达到稳态。

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