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首页> 外文期刊>Biological psychiatry >Conserved interneuron-specific ErbB4 expression in frontal cortex of rodents, monkeys, and humans: implications for schizophrenia.
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Conserved interneuron-specific ErbB4 expression in frontal cortex of rodents, monkeys, and humans: implications for schizophrenia.

机译:啮齿动物,猴子和人类的额叶皮层中保守的神经元特异性ErbB4表达:对精神分裂症的影响。

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BACKGROUND: Neuregulin-1 and ErbB4 are genetically associated with schizophrenia, and detailed knowledge of the cellular and subcellular localization of ErbB4 is important for understanding how neuregulin-1 regulates neuronal network activity and behavior. Expression of ErbB4 is restricted to interneurons in the rodent hippocampus and cortex. However, controversy remains about the cellular expression pattern in primate brain and its subcellular distribution in postsynaptic somatodendritic locations versus presynaptic terminals. METHODS: ErbB4 expression was analyzed in pyramidal cells and interneurons in the frontal cortex of five species: C57BL6 mice (n = 3), ErbB4/ mice (n = 2), Sprague-Dawley rats (n = 3), two macaque species (n = 3 + 2), and humans (normal control subjects, n = 2). We investigated 1) messenger RNA in mice, macaques, and humans; 2) protein expression in all species using highly specific monoclonal antibodies; and 3) specificity tests of several ErbB4 antibodies on brain samples (mouse, macaque, human). RESULTS: ErbB4 RNA is restricted to interneurons in the frontal cortex of mice. ErbB4 protein is undetectable in pyramidal cells of rodents, macaques, and human frontal cortex, whereas most interneurons positive for parvalbumin, calretinin, or cholecystokinin, but only a minority of calbindin-positive cells, co-express ErbB4 in macaques. Importantly, no presynaptic ErbB4 expression was detected in any species. CONCLUSIONS: The interneuron-selective somatodendritic expression of ErbB4 is consistent with a primary role of neuregulin-ErbB4 signaling in the postsynaptic modulation of gamma-aminobutyric acidergic function in rodents and primates. Our data validate the use of rodents to analyze effects of abnormal ErbB4 function as a means to model endophenotypes of psychiatric disorders.
机译:背景:神经调节蛋白1和ErbB4在遗传上与精神分裂症相关,对ErbB4的细胞和亚细胞定位的详细了解对于了解神经调节蛋白1如何调节神经元网络活动和行为很重要。 ErbB4的表达仅限于啮齿动物海马和皮层中的中间神经元。但是,关于灵长类动物大脑中的细胞表达模式及其在突触后躯体树突状位置相对于突触前末端的亚细胞分布的争论仍然存在。方法:分析了五种物种额叶皮层锥体细胞和中间神经元中ErbB4的表达:C57BL6小鼠(n = 3),ErbB4 /小鼠(n = 2),Sprague-Dawley大鼠(n = 3),两种猕猴( n = 3 + 2)和人类(正常对照组,n = 2)。我们研究了1)小鼠,猕猴和人类中的信使RNA; 2)使用高度特异性的单克隆抗体在所有物种中表达蛋白质; 3)几种ErbB4抗体对大脑样本(小鼠,猕猴,人)的特异性测试。结果:ErbB4 RNA局限于小鼠额叶皮层的中间神经元。 ErbB4蛋白在啮齿动物,猕猴和人额叶皮层的锥体细胞中无法检测到,而大多数中间神经元对小白蛋白,钙调蛋白或胆囊收缩素呈阳性,但只有少数钙结合蛋白阳性细胞在猕猴中共表达ErbB4。重要的是,在任何物种中均未检测到突触前的ErbB4表达。结论:ErbB4的神经元间选择性体树突状表达与啮齿动物和灵长类动物的γ-氨基丁酸酸能功能的突触后调节中的神经调节蛋白-ErbB4信号的主要作用是一致的。我们的数据验证了啮齿动物的使用,以分析异常ErbB4功能的影响,以此作为对精神疾病内表型进行建模的手段。

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