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Exploring the Wnt signaling pathway in schizophrenia and bipolar disorder

机译:探索精神分裂症和双相情感障碍的Wnt信号通路

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摘要

The Wnt signaling pathway plays a crucial role in neurodevelopment and in regulating the function and structure of the adult nervous system. Schizophrenia (SCZ) and bipolar disorder (BD) are severe mental disorders with evidence of subtle neurodevelopmental, structural and functional neuronal abnormalities. We aimed to elucidate the role of aberrant regulation of the Wnt system in these disorders by evaluating plasma levels of secreted Wnt modulators in patients (SCZ = 551 and BD = 246) and healthy controls (HCs = 639) using enzyme immune-assay. We also investigated the expression of 141 Wnt-related genes in whole blood in a subsample (SCZ = 338, BD = 241, and HCs = 263) using microarray analysis. Both SCZ and BD had dysregulated mRNA expression of Wnt-related genes favoring attenuated canonical (beta-catenin-dependent) signaling, and there were also indices of enhanced non-canonical Wnt signaling. In particular, FZD7, which may activate all Wnt pathways, but favors non-canonical signaling, and NFATc3, a downstream transcription factor and readout of the non-canonical Wnt/Ca2+ pathway, were significantly increased in SCZ and BD (p < 3 × 10−4). Furthermore, patients had lower plasma levels of soluble dickkopf 1 and sclerostin (p < 0.01) compared with HC. Our findings suggest that SCZ and BD are characterized by abnormal Wnt gene expression and plasma protein levels, and we propose that drugs targeting the Wnt pathway may have a role in the treatment of severe mental disorders.
机译:Wnt信号通路在神经发育以及调节成人神经系统的功能和结构中起着至关重要的作用。精神分裂症(SCZ)和躁郁症(BD)是严重的精神障碍,具有微妙的神经发育,结构和功能性神经元异常的证据。我们的目的是通过酶免疫测定评估患者(SCZ = 551和BD 246)和健康对照(HCs = 639)中分泌的Wnt调节剂的血浆水平,从而阐明Wnt系统异常调节在这些疾病中的作用。我们还使用微阵列分析研究了子样本(SCZ = 338,BD = 241和HCs = 263)在全血中​​141个Wnt相关基因的表达。 SCZ和BD都有Wnt相关基因的mRNA表达失调,有利于减弱的规范性(β-catenin依赖性)信号传导,并且还有增强的非规范性Wnt信号传导的指标。特别是,可能激活所有Wnt途径但有利于非经典信号传导的FZD7,NFATc3(下游转录因子和非经典Wnt / Ca 2 + 途径的读数)显着增加。在SCZ和BD中(p <3×10 −4 )。此外,与HC相比,患者血浆中的可溶性dickkopf 1和硬化蛋白的血浆水平较低(p <0.01)。我们的发现表明SCZ和BD的特征在于Wnt基因表达异常和血浆蛋白水平异常,并且我们建议靶向Wnt途径的药物可能在治疗严重精神障碍中起作用。

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