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首页> 外文期刊>Brain stimulation >Mapping brain regions in which deep brain stimulation affects schizophrenia-like behavior in two rat models of schizophrenia
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Mapping brain regions in which deep brain stimulation affects schizophrenia-like behavior in two rat models of schizophrenia

机译:在两个精神分裂症大鼠模型中绘制大脑深部刺激会影响精神分裂症样行为的大脑区域的图

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摘要

Background and Objectives: The development of more efficient treatment remains a major unmet need in the realm of schizophrenia disease. Using the maternal immune stimulation and the pubertal cannabinoid administration rat model of schizophrenia, the present study aimed at testing the hypothesis that deep brain stimulation (DBS) serves as a novel therapeutic technique for this disorder. Methods: Adult offspring of dams, treated with the immune activating agent poly I:C (4 mg/kg, n = 50) or saline (n = 50), underwent bilateral stereotactic electrode implantation into one of the following brain regions: subthalamic nucleus (STN, n = 12/10), entopeduncularis nucleus (EP, n = 10/11), globus pallidus (GP, n = 10/10), medial prefrontal cortex (mPFC, n = 8/8), or dorsomedial thalamus (DM, n = 10/11). Adult rats treated with the CB1 receptor agonist WIN 55,212-2 (WIN, n = 16) or saline (n = 12) during puberty were bilaterally implanted with electrodes into either the mPFC (n = 8/6) or the DM (n = 8/6). After a post-operative recovery period of one week, all rats were tested on a well-established cross-species phenomenon that is disrupted in schizophrenia, the pre-pulse inhibition (PPI) of the acoustic startle reflex (ASR) under different DBS conditions. Results: Poly I:C induced deficits in PPI of the ASR were normalized upon DBS. DBS effects depended on both stimulation target and stimulation parameters. Most prominent effects were found under DBS at high frequencies in the mPFC and DM. These effects were replicated in the pubertal WIN administration rat model of schizophrenia. Conclusions: Brain regions, in which DBS normalized PPI deficits, might be of therapeutic relevance to the treatment of schizophrenia. Results imply that DBS could be considered a plausible therapeutic technique in the realm of schizophrenia disease.
机译:背景与目的:开发更有效的治疗方法仍然是精神分裂症疾病领域的主要未满足需求。使用母亲的免疫刺激和精神分裂症的青春期大麻素给药大鼠模型,本研究旨在检验关于深部脑刺激(DBS)用作这种疾病的一种新型治疗技术的假设。方法:用免疫激活剂poly I:C(4 mg / kg,n = 50)或生理盐水(n = 50)处理的水坝成年后代,将双侧立体定向电极植入以下大脑区域之一:丘脑下核(STN,n = 12/10),上皮髓核(EP,n = 10/11),苍白球(GP,n = 10/10),内侧前额叶皮层(mPFC,n = 8/8)或丘脑背侧丘脑(DM,n = 10/11)。在青春期用CB1受体激动剂WIN 55,212-2(WIN,n = 16)或生理盐水(n = 12)处理的成年大鼠被双边植入电极到mPFC(n = 8/6)或DM(n = 8/6)。术后一周恢复期后,对所有大鼠进行均一的建立的跨物种现象测试,该现象在精神分裂症,在不同DBS条件下的听觉惊吓反射(ASR)的脉冲前抑制(PPI)受到破坏。结果:Poly I:C诱导的ASR PPI缺陷通过DBS进行了标准化。 DBS效应取决于刺激目标和刺激参数。在mPFC和DM中,在DBS的高频下发现了最显着的效果。这些作用在精神分裂症的青春期WIN给药大鼠模型中复制。结论:DBS使PPI缺陷正常化的大脑区域可能与精神分裂症的治疗相关。结果表明,DBS在精神分裂症疾病领域可以被视为一种可行的治疗技术。

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