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溶质载体家族39成员8基因(SLC39A8)的p.(Ala391Thr)与较差的认知能力相关:一项针对精神分裂症患者和英国普通人群的横断面研究

SLC39A8.p.(Ala391Thr) is associated with poorer cognitive ability: a cross-sectional study of schizophrenia and the general UK population.

作者信息

Smart Sophie E, Legge Sophie E, Fenner Eilidh, Pardiñas Antonio F, Woolway Grace, Lynham Amy J, Escott-Price Valentina, Hall Jeremy, Wilkinson Lawrence, Holmans Peter, O'Donovan Michael C, Owen Michael J, Walters James T R

机构信息

Centre for Neuropsychiatric Genetics and Genomics, Division of Psychological Medicine and Clinical Neurosciences, Cardiff University, Cardiff, UK.

Neuroscience and Mental Health Innovation Institute, Division of Psychological Medicine and Clinical Neurosciences, Cardiff University, Cardiff, UK.

出版信息

medRxiv. 2024 Sep 19:2024.09.18.24313865. doi: 10.1101/2024.09.18.24313865.

Abstract

The missense SNP NC_000004.12:g.102267552C>T (SLC39A8.p.(Ala391Thr), rs13107325) in , which encodes a zinc transporter, has been linked to schizophrenia and is the likely causal variant for one of the genome-wide association loci associated with the disorder. We tested whether the schizophrenia-risk allele at p.(Ala391Thr) was associated with schizophrenia-related phenotypes, including positive, negative, and disorganised symptoms, cognitive ability, educational attainment, and age of psychosis onset, within three schizophrenia cohorts (combined N=1,232) and, with equivalent phenotypes, in a sample of population controls (UK Biobank, N=355,069). We used regression analyses controlling for age, sex, and population stratification. Within the schizophrenia cohorts, after correction for multiple testing, p.(Ala391Thr) was not significantly associated with any schizophrenia-related phenotypes. In the unaffected participants from the UK Biobank, the schizophrenia-risk allele at p.(Ala391Thr) was associated with significantly poorer cognitive ability and fluid intelligence, a lower probability of obtaining GCSEs or a degree-level qualification, and fewer years in education. There was no association between p.(Ala391Thr) and self-reported psychotic experiences in this cohort. The schizophrenia-risk allele was associated with poorer cognitive ability, but not psychotic experiences, in a volunteer sample drawn from of the general population. To determine whether p.(Ala391Thr) is associated with cognitive phenotypes in people with schizophrenia, and to understand the role of p.(Ala391Thr) in the aetiology of cognitive impairment in schizophrenia, larger independent samples are required.

摘要

位于 上的错义单核苷酸多态性(SNP)NC_000004.12:g.102267552C>T(SLC39A8.p.(Ala391Thr),rs13107325)编码一种锌转运蛋白,该多态性与精神分裂症相关,并且可能是与该疾病相关的全基因组关联位点之一的因果变异。我们在三个精神分裂症队列(合并样本量 N = 1232)中测试了 p.(Ala391Thr) 处的精神分裂症风险等位基因是否与精神分裂症相关表型有关,这些表型包括阳性、阴性和紊乱症状、认知能力、教育程度以及精神病发作年龄;同时,在一个人群对照样本(英国生物银行,N = 355,069)中测试了其与同等表型的关系。我们使用了控制年龄、性别和人群分层的回归分析。在精神分裂症队列中,经过多重检验校正后,p.(Ala391Thr) 与任何精神分裂症相关表型均无显著关联。在英国生物银行的未受影响参与者中,p.(Ala391Thr) 处的精神分裂症风险等位基因与显著较差的认知能力和流体智力、获得普通中等教育证书(GCSE)或学位水平资格的概率较低以及受教育年限较少有关。在该队列中,p.(Ala391Thr) 与自我报告的精神病体验之间没有关联。在从普通人群中抽取的志愿者样本中,精神分裂症风险等位基因与较差的认知能力有关,但与精神病体验无关。为了确定 p.(Ala391Thr) 是否与精神分裂症患者的认知表型相关,并了解 p.(Ala391Thr) 在精神分裂症认知障碍病因学中的作用,需要更大的独立样本。

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