PGP Regulation of Antipsychotic Exposure and Effects

PGP 抗精神病药物暴露和作用的调节

• 批准号: 7175428
• 负责人: C Lindsay LINDSAY DEVANE
• 金额: $ 24.92万
• 依托单位: MEDICAL UNIVERSITY OF SOUTH CAROLINA
• 依托单位国家: 美国
• 财政年份: 2005
• 资助国家: 美国
• 起止时间: 2005-02-14 至 2009-01-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7175428
• 关键词: ABCB1 gene; Acute; Animal Behavior; Animal Experiments; Animals; Antipsychotic Agents; Area; Bile fluid; Blood - brain barrier anatomy; Brain; Class; Clozapine; Control Animal; Control Groups; Data; Dopamine; Dose; Drug Delivery Systems; Drug Kinetics; Drug or chemical Tissue Distribution; Endothelial Cells; Exposure to; Family; Future; Genes; Goals; Guidelines; HIV Infections; Human; Injection of therapeutic agent; Intervention; Intestines; Measures; Medial; Mentally Ill Persons; Microdialysis; Motor; Mus; Neuraxis; Neurotransmitters; Organ; Outcome; P-Glycoprotein; P-Glycoproteins; Pathway interactions; Patients; Peripheral; Pharmaceutical Preparations; Pharmacodynamics; Pharmacotherapy; Placenta; Plasma; Play; Prefrontal Cortex; Psychiatry; Range; Rattus; Regulation; Research; Research Design; Research Personnel; Risperidone; Role; Sampling; Site; Surrogate Markers; Symptoms; Testing; Tissues; Transgenic Mice; Transgenic Organisms; Urine; aripiprazole; atypical antipsychotic; behavior measurement; clinical efficacy; drug distribution; drug efficacy; extracellular; improved; in vivo; inhibitor/antagonist; innovation; intraperitoneal; neurotransmitter release; novel; novel therapeutics; olanzapine; oncology; programs; putamen; quetiapine; research study; response; severe mental illness; translational study; uptake; ziprasidone

DESCRIPTION (provided by applicant): The proposed investigator-initiated project is a revision of a previous application that received an encouraging initial review. The application focuses on P-glycoprotein (P-gp) as an important modulator of brain access and, therefore, pharmacologic effects of antipsychotic drugs. Antipsychotic drugs (APD) are the primary pharmacological intervention in the treatment of severe mental illness with psychotic symptoms. The proposed animal studies are designed to produce data that may contribute to improving the outcome of pharmacotherapy with APD. While the pathways of elimination of the APD have been defined, only sparse data exist on the role of drug transporters in their disposition and effects. The most widely studied gene of the ABC cassette family of transporters, ABCB1 (also known as MDR1), is highly polymorphic and encodes for P-gp. P-gp plays a protective role for major organs by effluxing its substrates into the intestinal lumen, bile, urine, and by limiting their passage across the placenta and accumulation in the central nervous system. We will test the hypothesis that P-gp is an important modulator of brain access and pharmacologic effects of a subclass of APD, the atypicals. Similarly, we will test whether inhibition and induction of P-gp in the endothelial cells at the blood brain barrier increases or decreases, respectively, the brain exposure to, and effects of, APD. The specific aims are: (i) to evaluate the atypical APD as substrates of P-gp using transgenic mice; (ii) to determine the effects of P-gp inhibition and induction on plasma and tissue concentrations of APD; (iii) to assess neurotransmitter changes in the brain of P-gp inhibited animals using extracellular microdialysis of dopamine; and (iv) to measure behavioral changes in rats accompanying P-gp inhibition that are predictive of antipsychotic efficacy. This novel data may potentially guide future human trials to improve APD efficacy and/or tolerability with use of adjunctive P-gp modulators. The results of this research will provide support for translational studies in humans to refine treatment guidelines for the use of this class of medications in severely mentally ill patients.

描述（由申请人提供）：拟议的仲裁员发起的项目是对先前收到令人鼓舞的初步审查的申请的修订。该应用程序的重点是P-糖蛋白（P-gp）作为一个重要的调制器的大脑访问，因此，抗精神病药物的药理作用。抗精神病药物（APD）是治疗伴有精神病性症状的严重精神疾病的主要药物干预。拟定的动物研究旨在产生可能有助于改善APD药物治疗结局的数据。虽然已经确定了APD的消除途径，但关于药物转运蛋白在其处置和作用中的作用的数据很少。ABC盒转运蛋白家族中研究最广泛的基因ABCB 1（也称为MDR 1）具有高度多态性，编码P-gp。P-gp通过将其底物排出到肠腔、胆汁、尿液中，并通过限制其穿过胎盘和在中枢神经系统中蓄积，对主要器官起保护作用。我们将检验P-gp是脑通路的重要调节剂和APD亚类药物的药理作用的假设。同样，我们将测试血脑屏障内皮细胞中P-gp的抑制和诱导是否分别增加或减少脑暴露于APD和APD的影响。具体目标是：（i）使用转基因小鼠评价作为P-gp底物的非典型APD;（ii）确定P-gp抑制和诱导对APD血浆和组织浓度的影响;（iii）使用多巴胺的细胞外微透析评估P-gp抑制动物脑中神经递质的变化;（iv）测量伴随P-gp抑制的大鼠中预测抗精神病疗效的行为变化。这一新的数据可能会指导未来的人体试验，以改善APD的疗效和/或耐受性与使用连续的P-gp调节剂。这项研究的结果将为人类的转化研究提供支持，以完善在严重精神病患者中使用这类药物的治疗指南。