双相情感障碍
全基因组关联研究
多基因风险评分
精神分裂症(面向对象编程)
维加维斯
狂躁
遗传关联
基因座(遗传学)
遗传学
精神科
医学
生物
单核苷酸多态性
基因型
基因
心情
作者
Douglas M. Ruderfer,Ayman H. Fanous,Stephan Ripke,Andrew McQuillin,Richard Amdur,Pablo V. Gejman,Michael O’Donovan,Ole A. Andreassen,Srdjan Djurovic,Christina M. Hultman,John R. Kelsoe,Stéphane Jamain,Mikael Landén,Marion Leboyer,Vishwajit L. Nimgaonkar,John I. Nürnberger,Jordan W. Smoller,Nick Craddock,Aiden Corvin,Patrick F. Sullivan
摘要
Bipolar disorder and schizophrenia are two often severe disorders with high heritabilities. Recent studies have demonstrated a large overlap of genetic risk loci between these disorders but diagnostic and molecular distinctions still remain. Here, we perform a combined genome-wide association study (GWAS) of 19 779 bipolar disorder (BP) and schizophrenia (SCZ) cases versus 19 423 controls, in addition to a direct comparison GWAS of 7129 SCZ cases versus 9252 BP cases. In our case-control analysis, we identify five previously identified regions reaching genome-wide significance (CACNA1C, IFI44L, MHC, TRANK1 and MAD1L1) and a novel locus near PIK3C2A. We create a polygenic risk score that is significantly different between BP and SCZ and show a significant correlation between a BP polygenic risk score and the clinical dimension of mania in SCZ patients. Our results indicate that first, combining diseases with similar genetic risk profiles improves power to detect shared risk loci and second, that future direct comparisons of BP and SCZ are likely to identify loci with significant differential effects. Identifying these loci should aid in the fundamental understanding of how these diseases differ biologically. These findings also indicate that combining clinical symptom dimensions and polygenic signatures could provide additional information that may someday be used clinically.
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