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慢性亚麻醉 NMDA 拮抗剂治疗后海马区的副钙蛋白丢失具有年龄依赖性:对 NMDA 功能低下建模的影响。

Parvalbumin Loss Following Chronic Sub-Anesthetic NMDA Antagonist Treatment is Age-Dependent in the Hippocampus: Implications for Modeling NMDA Hypofunction.

机构信息

Department of Psychology, Division of Behavioral Neuroscience, 406 Babbidge Road Unit 1020, University of Connecticut, Storrs, CT 06269, USA; Department of Psychology, 360 Huntington Ave NI 125, Northeastern University, Boston, MA 02115, USA.

Department of Psychology, Division of Behavioral Neuroscience, 406 Babbidge Road Unit 1020, University of Connecticut, Storrs, CT 06269, USA.

出版信息

Neuroscience. 2018 Nov 21;393:73-82. doi: 10.1016/j.neuroscience.2018.09.031. Epub 2018 Oct 6.

DOI:10.1016/j.neuroscience.2018.09.031
PMID:30296474
Abstract

A marked decrease in parvalbumin (PV), a calcium-binding protein specific to a subset of GABAergic neurons, is a consistent finding in postmortem schizophrenic brain tissue. This reduction is selective to PV and is regionally specific, occurring primarily in the prefrontal cortex and hippocampus (HPC) of patients. Rodent models of NMDA receptor hypofunction utilizing NMDA antagonist treatments - e.g. ketamine (KET) - show schizophrenia-like cognitive and behavioral impairments with parallel changes in PV. While decreased PV is considered a hallmark of neuropathology in schizophrenia, previous work elucidating the effects of KET administration on PV are contradictory, with findings suggesting decreased, increased, or no change in PV expression. Upon close examination of the procedures used across studies, there are two primary inconsistencies, including: (1) the age of animals used; and (2) the timeline of post-treatment tissue collection. To better understand whether these key differences impact observed PV changes, the present study investigated the impact of age and time of sacrifice on chronic KET-induced PV changes in the neocortex and HPC. Our findings suggest an effect of age, but not sacrifice timeline, on PV cell count following 14 days of sub-anesthetic KET treatment. We provide evidence that 1-month-old rats exhibit a significant KET-induced HPC PV decrease, while adult rats show a modest increase in HPC PV following chronic KET. Taken together, we propose that PV is a dynamic marker, and that changes in cell counts - and their interpretation - following NDMA antagonist treatment should be considered in the context of age.

摘要

钙结合蛋白 parvalbumin(PV)在 GABA 能神经元亚群中特异性表达,其在精神分裂症死后脑组织中的表达明显减少,这是一个一致的发现。这种减少是 PV 特异性的,具有区域性特异性,主要发生在患者的前额叶皮层和海马体(HPC)。利用 NMDA 拮抗剂治疗(如氯胺酮(KET))建立的 NMDA 受体功能低下的啮齿动物模型表现出类似精神分裂症的认知和行为障碍,同时伴随着 PV 的平行变化。虽然 PV 减少被认为是精神分裂症神经病理学的标志,但先前阐明 KET 给药对 PV 影响的研究结果存在矛盾,发现提示 PV 表达减少、增加或没有变化。在仔细检查了跨研究使用的程序后,发现有两个主要的不一致之处,包括:(1)动物的年龄;(2)治疗后组织采集的时间。为了更好地了解这些关键差异是否会影响观察到的 PV 变化,本研究调查了年龄和处死时间对慢性 KET 诱导的新皮层和 HPC 中 PV 变化的影响。我们的研究结果表明,年龄对 KET 治疗 14 天后的 PV 细胞计数有影响,但处死时间没有影响。我们提供的证据表明,1 个月大的大鼠表现出 HPC 中 KET 诱导的 PV 明显减少,而成年大鼠在慢性 KET 后 HPC 中 PV 略有增加。综上所述,我们提出 PV 是一个动态标志物,NMDA 拮抗剂治疗后细胞计数的变化及其解释应考虑到年龄因素。

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