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Immune system disturbances in schizophrenia

机译:精神分裂症的免疫系统紊乱

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摘要

Epidemiological, genetic, transcriptome, postmortem, peripheral biomarker, and therapeutic studies of schizophrenia all point to a dysregulation of both innate and adaptive immune systems in the disease, and it is likely that these immune changes actively contribute to disease symptoms. Gene expression disturbances in the brain of subjects with schizophrenia show complex, region-specific changes with consistently replicated and potentially interdependent induction of serpin peptidase inhibitor, clade A member 3 (SERPINA3) and interferon inducible transmembrane protein (IFITM) family transcripts in the prefrontal cortex. Recent data suggest that IFITM3 expression is a critical mediator of maternal immune activation. Because the IFITM gene family is primarily expressed in the endothelial cells and meninges, and because the meninges play a critical role in interneuron development, we suggest that these two non-neuronal cell populations might play an important role in the disease pathophysiology. Finally, we propose that IFITM3 in particular might be a novel, appealing, knowledge-based drug target for treatment of schizophrenia.
机译:精神分裂症的流行病学,遗传学,转录组,验尸,外周生物标志物和治疗研究均表明该疾病先天免疫系统和适应性免疫系统均失调,这些免疫变化很可能积极地导致疾病症状。精神分裂症患者大脑中的基因表达障碍表现出复杂的,区域特定的变化,并在前额叶皮层中持续复制并可能相互依赖地诱导丝氨酸蛋白酶抑制肽酶抑制剂,进化枝A成员3(SERPINA3)和干扰素诱导跨膜蛋白(IFITM)家族转录物。最新数据表明,IFITM3表达是孕产妇免疫激活的关键介质。因为IFITM基因家族主要在内皮细胞和脑膜中表达,并且由于脑膜在中神经元发育中起关键作用,所以我们建议这两个非神经元细胞群可能在疾病的病理生理学中起重要作用。最后,我们建议特别是IFITM3可能是治疗精神分裂症的一种新颖的,有吸引力的,基于知识的药物靶标。

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