Impact of the Reelin signaling cascade (ligands-receptors-adaptor complex) on cognition in schizophrenia.

Phebe Verbrugghe, Sonja Bouwer, Steven Wiltshire, Kim Carter, David Chandler, Matthew Cooper, Bharti Morar, Muhammad F M Razif, Anjali Henders, Johanna C Badcock, Milan Dragovic, Vaughan Carr, Osvaldo P Almeida, Leon Flicker, Grant Montgomery, Assen Jablensky, Luba Kalaydjieva
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引用次数: 30

Abstract

Our previous neurocognitive studies of schizophrenia outlined two clusters of affected subjects--cognitively spared (CS) and cognitive deficit (CD), the latter's characteristics pointing to developmental origins and impaired synaptic plasticity. Here we investigate the contribution of polymorphisms in major regulators of these processes to susceptibility to schizophrenia and to CD in patients. We examine variation in genes encoding proteins at the gateway of Reelin signaling: ligands RELN and APOE, their common receptors APOER2 and VLDLR, and adaptor DAB1. Association analysis with disease outcome and cognitive performance in the Western Australian Family Study of Schizophrenia (WAFSS) was followed by replication analysis in the Australian Schizophrenia Research Bank (ASRB) and in the Health in Men Study (HIMS) of normal aging males. In the WAFSS sample, we observed significant association of APOE, APOER2, VLDLR, and DAB1 SNPs with disease outcome in the case-control and CD-control datasets, and with pre-morbid intelligence and verbal memory in cases. HIMS replication analysis supported rs439401 (APOE regulatory region), and rs2297660 and rs3737983 (APOER2), with an effect on memory performance in normal aging subjects consistent with the findings in schizophrenia cases. APOER2 gene expression analysis revealed lower transcript levels in lymphoblastoid cells from cognitively impaired schizophrenia patients of the alternatively spliced exon 19, mediating Reelin signaling and synaptic plasticity in the adult brain. ASRB replication analysis produced marginally significant results, possibly reflecting a recruitment strategy biased toward CS patients. The data suggest a contribution of neurodevelopmental/synaptic plasticity genes to cognitive impairment in schizophrenia.

Reelin信号级联(配体-受体-受体复合体)对精神分裂症认知的影响。
我们之前对精神分裂症的神经认知研究概述了两类受影响的受试者——认知空白(CS)和认知缺陷(CD),后者的特征指向发育起源和突触可塑性受损。在这里,我们研究了这些过程的主要调节因子的多态性对精神分裂症和乳糜泻患者易感性的贡献。我们研究了Reelin信号通路蛋白编码基因的变异:配体RELN和APOE,它们的共同受体APOER2和VLDLR,以及适配器DAB1。在西澳大利亚精神分裂症家庭研究(WAFSS)中进行了与疾病结局和认知表现的关联分析,随后在澳大利亚精神分裂症研究银行(ASRB)和正常老年男性健康研究(HIMS)中进行了重复分析。在WAFSS样本中,我们观察到APOE、APOER2、VLDLR和DAB1 snp与病例对照和cd对照数据集中的疾病结局以及病例的发病前智力和言语记忆有显著关联。HIMS复制分析支持rs439401 (APOE调控区)、rs2297660和rs3737983 (APOER2)对正常衰老受试者记忆表现的影响,这与精神分裂症患者的研究结果一致。APOER2基因表达分析显示,在认知障碍精神分裂症患者的淋巴母细胞样细胞中,介导Reelin信号传导和成人大脑突触可塑性的选择性剪接外显子19的转录水平较低。ASRB复制分析产生了边际显著的结果,可能反映了偏向于CS患者的招募策略。这些数据表明神经发育/突触可塑性基因与精神分裂症患者的认知障碍有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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