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RBM12 截断突变与精神病有关。

Truncating mutations in RBM12 are associated with psychosis.

机构信息

deCODE Genetics/Amgen, Reykjavik, Iceland.

National Institute for Health and Welfare (THL), Helsinki, Finland.

出版信息

Nat Genet. 2017 Aug;49(8):1251-1254. doi: 10.1038/ng.3894. Epub 2017 Jun 19.

Abstract

Thus far, a handful of highly penetrant mutations conferring risk of psychosis have been discovered. Here we used whole-genome sequencing and long-range phasing to investigate an Icelandic kindred containing ten individuals with psychosis (schizophrenia, schizoaffective disorder or psychotic bipolar disorder). We found that all affected individuals carry RBM12 (RNA-binding-motif protein 12) c.2377G>T (P = 2.2 × 10), a nonsense mutation that results in the production of a truncated protein lacking a predicted RNA-recognition motif. We replicated the association in a Finnish family in which a second RBM12 truncating mutation (c.2532delT) segregates with psychosis (P = 0.020). c.2377G>T is not fully penetrant for psychosis; however, we found that carriers unaffected by psychosis resemble patients with schizophrenia in their non-psychotic psychiatric disorder and neuropsychological test profile (P = 0.0043) as well as in their life outcomes (including an increased chance of receiving disability benefits, P = 0.011). As RBM12 has not previously been linked to psychosis, this work provides new insight into psychiatric disease.

摘要

迄今为止,已经发现了少数一些具有高穿透性的突变,它们会增加患精神病的风险。在这里,我们使用全基因组测序和长程相位分析来研究一个冰岛家族,该家族中有十名患有精神病(精神分裂症、分裂情感障碍或精神病性双相情感障碍)的个体。我们发现所有受影响的个体都携带 RBM12(RNA 结合基序蛋白 12)c.2377G>T(P = 2.2×10),这是一种无义突变,导致产生一种缺少预测 RNA 识别基序的截断蛋白。我们在一个芬兰家族中复制了这种关联,该家族中的另一个 RBM12 截断突变(c.2532delT)与精神病一起遗传(P = 0.020)。c.2377G>T 并不是精神病的完全外显率;然而,我们发现,未受精神病影响的携带者在非精神病性精神障碍和神经心理学测试特征(P = 0.0043)以及生活结果(包括获得残疾福利的机会增加,P = 0.011)方面与精神分裂症患者相似。由于 RBM12 以前与精神病没有联系,这项工作为精神疾病提供了新的见解。

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