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Bipolar disorder risk gene FOXO6 modulates negative symptoms in schizophrenia: a neuroimaging genetics study

机译:双极性障碍风险基因FOXO6调节精神分裂症中的阴性症状:神经影像学遗传学研究

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Background: Despite being diagnostically associated uniquely with schizophrenia, negative symptoms are also observed in bipolar disorder (BD). Genome-wide association studies (GWAS) have uncovered a number of shared risk genes between schizophrenia and BD. The objectives of this study were to examine whether previously identified risk genes for BD are associated with negative symptom severity within a first-episode schizophrenia (FES) cohort and to examine whether such genes influence brain morphology. Methods: Patients experiencing FES were genotyped for 21 previously identified BD risk genes; a series of univariate analyses of covariance examined the association between negative symptom severity, as measured using the Scale for the Assessment of Negative Symptoms (SANS), and genotype. A subset of participants underwent a structural 1.5 T MRI T-1 scan, analyzed for surface area and cortical thickness changes via the CIVET pipeline and LPBA40 atlas. Results: We included 133 patients with FES in our analysis; 61 of them underwent structural MRI. We observed a significant association between negative symptom severity and the BD risk gene FOXO6 (rs4660531). Individuals with the CC genotype presented significantly higher negative symptoms (Cohen d = 0.46, F = 5.854, p = 0.017) and significantly smaller surface area within the right middle orbitofrontal gyrus (Cohen d = 0.69, F = 7.289, p = 0.009) than carriers of allele A. Limitations: Limitations of this study include its modest sample size and lack of a control sample. Conclusion: Lacking the FOXO6 risk allele was associated with an increase in negative symptoms and surface area reduction in the right orbitofrontal gyrus - an area previously associated with negative symptoms - suggesting that presence of the FOXO6 risk allele confers resistance against negative symptoms and associated neuroanatomical changes in individuals with FES.
机译:背景:尽管诊断上与精神分裂症唯一相关,但双相情感障碍(BD)中也观察到阴性症状。全基因组关联研究(GWAS)发现了精神分裂症和BD之间的一些共同风险基因。本研究的目的是在首发精神分裂症(FES)队列中检查先前确定的BD风险基因是否与阴性症状严重程度相关,并检查这些基因是否影响大脑形态。方法:对FES患者进行21个先前确定的BD风险基因的基因分型;一系列单变量协方差分析检验了阴性症状严重程度(使用阴性症状评估量表(SANS)测量)与基因型之间的关联。一部分参与者接受了结构1.5 T MRI T-1扫描,通过麝香猫管道和LPBA40图谱分析表面积和皮质厚度的变化。结果:我们分析了133例FES患者;其中61人接受了结构MRI检查。我们观察到阴性症状严重程度与BD风险基因FOXO6(rs4660531)之间存在显著相关性。CC基因型个体的阴性症状显著高于等位基因A携带者(Cohen d=0.46,F=5.854,p=0.017),右眶额中回的表面积显著小于等位基因A携带者(Cohen d=0.69,F=7.289,p=0.009)。结论:缺乏FOXO6风险等位基因与阴性症状的增加和右眶额回表面积的减少有关,这一区域以前与阴性症状有关,表明FOXO6风险等位基因的存在使FES患者对阴性症状和相关神经解剖学改变产生抵抗。

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