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抗精神病药物的使用与人类尸检大脑标本背外侧前额叶皮质中 CRP40/ mortalin mRNA 的表达相关。

Antipsychotic drug use is correlated with CRP40/mortalin mRNA expression in the dorsolateral prefrontal cortex of human postmortem brain specimens.

机构信息

Department of Psychiatry and Behavioural Neurosciences, McMaster University, Hamilton, Ontario, Canada.

出版信息

Schizophr Res. 2010 Jun;119(1-3):228-31. doi: 10.1016/j.schres.2009.12.039. Epub 2010 Jan 25.

DOI:10.1016/j.schres.2009.12.039
PMID:20100649
Abstract

Heat shock proteins act as intracellular chaperones by assisting with proper protein folding in response to various cellular stresses. In doing so, these proteins protect the cell from unwanted protein aggregation, which in turn, plays an important role in the pathogenesis of numerous disorders. Previous reports from our laboratory have described a 40 kDa catecholamine regulated heat shock-like protein (CRP40), an alternate gene product of the 70 kDa mitochondrial heat shock protein, mortalin. CRP40 shares an intimate association with dopaminergic activity, specifically as it pertains to dopamine dysregulation in schizophrenia. This study investigates human CRP40/mortalin mRNA expression within dorsolateral prefrontal cortex postmortem specimens from normal control, schizophrenic and bipolar patients obtained from the Stanley Medical Research Institute. Real-time polymerase chain reaction was carried out for all patient samples (n=105; n=35 per group) in a blinded manner. No significant alterations in CRP40/mortalin mRNA expression levels were observed between control, bipolar and schizophrenic patients. However, multiple regression demonstrated a distinct positive correlation between CRP40/mortalin mRNA expression and lifetime use of antipsychotic drugs within the schizophrenic patient profile, after controlling for important confounding factors. Thus, the data suggest that human CRP40/mortalin is modulated by dopaminergic activity and may act to protect neurons from excess catecholamine activity in regions of the brain associated with psychosis.

摘要

热休克蛋白作为细胞内伴侣,通过在应对各种细胞应激时协助正确的蛋白质折叠来发挥作用。这样,这些蛋白质可以防止细胞内不受欢迎的蛋白质聚集,这反过来在许多疾病的发病机制中起着重要作用。我们实验室之前的报告描述了一种 40 kDa 的儿茶酚胺调节的热休克样蛋白 (CRP40),它是 70 kDa 线粒体热休克蛋白 mortalin 的另一种基因产物。CRP40 与多巴胺能活性密切相关,特别是与精神分裂症中的多巴胺失调有关。本研究调查了来自斯坦利医学研究所的正常对照、精神分裂症和双相障碍患者死后标本中人类 CRP40/mortalin mRNA 的表达。所有患者样本(n=105;每组 n=35)均以盲法进行实时聚合酶链反应。在对照、双相和精神分裂症患者之间,CRP40/mortalin mRNA 表达水平没有明显改变。然而,多元回归分析表明,在控制了重要的混杂因素后,CRP40/mortalin mRNA 表达与精神分裂症患者一生中使用抗精神病药物之间存在明显的正相关。因此,数据表明人类 CRP40/mortalin 受多巴胺能活性的调节,并且可能在与精神病相关的大脑区域中通过保护神经元免受过量儿茶酚胺活性的影响而起作用。

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Antipsychotic drug use is correlated with CRP40/mortalin mRNA expression in the dorsolateral prefrontal cortex of human postmortem brain specimens.抗精神病药物的使用与人类尸检大脑标本背外侧前额叶皮质中 CRP40/ mortalin mRNA 的表达相关。
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