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Transfer of disrupted-in-schizophrenia 1 aggregates between neuronal-like cells occurs in tunnelling nanotubes and is promoted by dopamine

机译:神经元样细胞之间的分裂型精神分裂症1聚集体的转移发生在隧穿纳米管中并由多巴胺促进

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摘要

The disrupted-in-schizophrenia 1 (DISC1) gene was identified as a genetic risk factor for chronic mental illnesses (CMI) such as schizophrenia, bipolar disorder and severe recurrent depression. Insoluble aggregated DISC1 variants were found in the cingular cortex of sporadic, i.e. non-genetic, CMI patients. This suggests protein pathology as a novel, additional pathogenic mechanism, further corroborated in a recent transgenic rat model presenting DISC1 aggregates. Since the potential role of aggregation of DISC1 in sporadic CMI is unknown, we investigated whether DISC1 undergoes aggregation in cell culture and could spread between neuronal cells in a prion-like manner, as shown for amyloid proteins in neurodegenerative diseases. Co-culture experiments between donor cells forming DISC1 aggregates and acceptor cells showed that 4.5% of acceptor cells contained donor-derived DISC1 aggregates, thus indicating an efficient transfer in vitro. DISC1 aggregates were found inside tunnelling nanotubes (TNTs) and transfer was enhanced by increasing TNT formation and notably by dopamine treatment, which also induces DISC1 aggregation. These data indicate that DISC1 aggregates can propagate between cells similarly to prions, thus providing some molecular basis for the role of protein pathology in CMI.
机译:精神分裂症1(DISC1)的基因被确定为慢性精神疾病(CMI)的遗传危险因素,例如精神分裂症,躁郁症和严重的反复抑郁症。在散发性即非遗传性CMI患者的扣带皮层中发现了不溶的聚集DISC1变体。这表明蛋白质病理学是一种新颖的,额外的致病机制,在最近呈现DISC1聚集体的转基因大鼠模型中得到了进一步证实。由于DISC1聚集在散发性CMI中的潜在作用尚不清楚,因此我们研究了DISC1是否在细胞培养物中发生聚集,并可能以a病毒样方式在神经元细胞之间传播,如神经变性疾病中的淀粉样蛋白所示。形成DISC1聚集体的供体细胞与受体细胞之间的共培养实验表明,4.5%的受体细胞含有供体衍生的DISC1聚集体,因此表明在体外有效转移。在隧道纳米管(TNT)内部发现DISC1聚集体,并且通过增加TNT的形成,特别是通过多巴胺处理,也可以诱导DISC1聚集,从而增强了转移。这些数据表明,DISC1聚集体可以像ions病毒一样在细胞之间传播,从而为蛋白质病理学在CMI中的作用提供了分子基础。

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