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首页> 外文期刊>Schizophrenia bulletin >Polygenic Risk for Schizophrenia Associated With Working Memory-related Prefrontal Brain Activation in Patients With Schizophrenia and Healthy Controls
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Polygenic Risk for Schizophrenia Associated With Working Memory-related Prefrontal Brain Activation in Patients With Schizophrenia and Healthy Controls

机译:与精神分裂症患者和健康对照者的工作记忆相关的前额叶脑激活相关的精神分裂症的多基因风险

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摘要

Schizophrenia is a highly heritable and polygenic disease, and identified common genetic variants have shown weak individual effects. Many studies have reported altered working memory (WM)-related brain activation in schizophrenia, preferentially in the frontal lobe. Such differences in brain activations could reflect inherited alterations possibly involved in the disease etiology, or rather secondary disease-related mechanisms. The use of polygenic risk scores (PGRS) based on a large number of risk polymorphisms with small effects is a valuable approach to examine the effect of cumulative genetic risk on brain functioning. This study examined the impact of cumulative genetic risk for schizophrenia on WM-related brain activations, assessed with functional magnetic resonance imaging. For each participant (63 schizophrenia patients and 118 healthy controls), we calculated a PGRS for schizophrenia based on 18 862 single-nucleotide polymorphism in a large multicenter genome-wide association study including 9146 schizophrenia patients and 12 111 controls, performed by the Psychiatric Genomics Consortium. As expected, the PGRS was significantly higher in patients compared with healthy controls. Further, the PGRS was related to differences in frontal lobe brain activation between high and low WM demand. Specifically, even in absence of main effects of diagnosis, increased PGRS was associated with decreased activation difference in the right middle-superior prefrontal cortex (BA 10/11) and the right inferior frontal gyrus (BA 45). This effect was seen in both cases and controls, and was not influenced by sex, age, or task performance. The findings support the notion of dysregulation of frontal lobe functioning as an inherited vulnerability factor in schizophrenia.
机译:精神分裂症是一种高度遗传和多基因的疾病,已确定的常见遗传变异显示出较弱的个体效应。许多研究报告说,精神分裂症,尤其是额叶的工作记忆(WM)相关的大脑激活发生了改变。脑部激活的这种差异可能反映出可能与疾病病因有关的遗传性变化,或与继发性疾病相关的机制有关。基于大量风险多态性且影响较小的多基因风险评分(PGRS)的使用,是检验累积遗传风险对脑功能的影响的有价值的方法。这项研究检查了精神分裂症的累积遗传风险对WM相关的大脑激活的影响,并通过功能磁共振成像进行了评估。对于每个参与者(63位精神分裂症患者和118位健康对照),我们根据一项由Psychiatric Genomics执行的大型多中心全基因组关联研究(包括9146位精神分裂症患者和12111位对照),基于18862个单核苷酸多态性计算了精神分裂症的PGRS财团。正如预期的那样,患者的PGRS明显高于健康对照组。此外,PGRS与高和低WM需求之间的额叶大脑激活差异有关。具体来说,即使没有诊断的主要影响,PGRS的增加也与右中上前额叶皮层(BA 10/11)和右下额叶回(BA 45)的激活差异降低有关。在病例和对照中均可见到这种效果,并且不受性别,年龄或工作表现的影响。这些发现支持了额叶失调作为精神分裂症的遗传易感因素的观点。

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