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Schizophrenia-Related Neural and Behavioral Phenotypes in Transgenic Mice Expressing Truncated Disc1

机译:精神分裂症相关的神经和行为表型在转基因小鼠中表达截短的Disc1。

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摘要

Disrupted-in-Schizophrenia-1 (DISC1), identified by positional cloning of a balanced translocation (1;11) with the breakpoint in intron 8 of a large Scottish pedigree, is associated with a range of neuropsychiatric disorders including schizophrenia. To model this mutation in mice, we have generated Disc1tr transgenic mice expressing 2 copies of truncated Disc1 encoding the first 8 exons using a bacterial artificial chromosome (BAC). With this partial simulation of the human situation, we have discovered a range of phenotypes including a series of novel features not previously reported. Disc1tr transgenic mice display enlarged lateral ventricles, reduced cerebral cortex, partial agenesis of the corpus callosum, and thinning of layers II/III with reduced neural proliferation at midneurogenesis. Parvalbumin GABAergic neurons are reduced in the hippocampus and medial prefrontal cortex, and displaced in the dorsolateral frontal cortex. In culture, transgenic neurons grow fewer and shorter neurites. Behaviorally, transgenic mice exhibit increased immobility and reduced vocalization in depression-related tests, and impairment in conditioning of latent inhibition. These abnormalities in Disc1tr transgenic mice are consistent with findings in severe schizophrenia.
机译:精神分裂症1(DISC1)是由苏格兰大谱系内含子8的内含子8断裂点的平衡易位(1; 11)的位置克隆确定的,与一系列神经精神疾病有关,包括精神分裂症。为了对小鼠中的这种突变进行建模,我们使用细菌人工染色体(BAC)生成了Disc1tr转基因小鼠,表达2个拷贝的截短Disc1编码前8个外显子。通过对人类状况的部分模拟,我们发现了一系列表型,包括一系列以前未曾报道的新颖特征。 Disc1tr转基因小鼠显示出侧脑室增大,大脑皮层减少,call体部分发育不全以及II / III层变薄,而在神经新生时神经增殖减少。小白蛋白GABA能神经元在海马和前额内侧皮层中减少,并在背外侧额叶皮层中移位。在文化中,转基因神经元生长的神经突越来越少。从行为上讲,转基因小鼠在与抑郁症相关的测试中显示出更高的固定性和发声能力,以及潜在抑制条件的损害。 Disc1tr转基因小鼠中的这些异常与严重精神分裂症中的发现一致。

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