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Neuropil contraction in relation to Complement C4 gene copy numbers in independent cohorts of adolescent-onset and young adult-onset schizophrenia patients–a pilot study

机译:在青少年和成年青年精神分裂症患者的独立队列中,神经纤维收缩与补体C4基因拷贝数的关系–一项初步研究

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A recent report suggested Complement 4 (C4A) gene copy numbers (GCN) as risk factors for schizophrenia. Rodent model showed association of C4 with synaptic pruning suggesting its pathophysiological significance (Sekar, A. et al. (2016)). We, therefore, predicted that C4A GCN would be positively correlated with neuropil contraction in the human brain among schizophrenia patients showing more prominent correlations in ventral regions among young adults and dorsal regions among adolescents since neuromaturation progresses dorsoventrally. Whole-brain, multi-voxel, in vivo phosphorus magnetic resonance spectroscopy (31P MRS) assessed neuropil changes by estimating levels of membrane phospholipid (MPL) precursors and catabolites. Increased MPL catabolites and/or decreased MPL precursors indexed neuropil contraction. Digital droplet PCR-based assay was used to estimate C4A and C4B GCN. We evaluated two independent cohorts (young adult-onset early-course schizophrenia (YASZ?=?15) and adolescent-onset schizophrenia (AOSZ?=?12) patients), and controls matched for each group, n =?22 and 15, respectively. Separate forward stepwise linear regression models with Akaike information Criterion were built for MPL catabolites and precursors. YASZ cohort : Consistent with the rodent model (Sekar, A. et al. 2016)), C4A GCN positively correlated with neuropil contraction (increased pruning/decreased formation) in the inferior frontal cortex and inferior parietal lobule. AOSZ cohort : C4A GCN positively correlated with neuropil contraction in the dorsolateral prefrontal cortex and thalamus. Exploratory analysis of C4B GCN showed positive correlation with neuropil contraction in the cerebellum and superior temporal gyrus among YASZ while AOSZ showed neuropil contraction in the prefrontal and subcortical structures. Thus, C4A and C4B GCN are associated with neuropil contraction in regions often associated with schizophrenia, and may be neuromaturationally dependent.
机译:最近的报告建议补体4(C4A)基因拷贝数(GCN)作为精神分裂症的危险因素。啮齿动物模型显示C4与突触修剪相关,表明其病理生理学意义(Sekar,A.et al。(2016))。因此,我们预测精神分裂症患者中的C4A GCN与人脑中的神经纤维收缩呈正相关,因为年轻人的腹侧神经成熟发展,因此在年轻人的腹侧区域和青少年的背侧区域显示出更明显的相关性。全脑,多体素体内磷磁共振波谱( 31 P MRS)通过估计膜磷脂(MPL)前体和分解代谢物的水平来评估神经纤维的变化。 MPL分解代谢物增加和/或MPL前体减少指示神经纤维收缩。基于数字液滴PCR的测定法用于评估C4A和C4B GCN。我们评估了两个独立的队列(年轻的成人发作早期精神分裂症(YASZ≥15)和青少年发作的精神分裂症(AOSZ≥12)患者),并且每组的对照组均匹配,n =≥22和15。分别。建立了具有Akaike信息准则的单独的逐步逐步线性回归模型,用于MPL分解代谢产物和前体。 YASZ队列:与啮齿动物模型一致(Sekar,A。等人,2016),C4A GCN与额额叶皮下和顶叶小叶中的神经纤维收缩(修剪/形成减少)呈正相关。 AOSZ队列:C4A GCN与背外侧前额叶皮层和丘脑的神经纤维收缩呈正相关。对C4B GCN的探索性分析显示,YASZ的小脑和颞上回的神经纤维收缩与正向神经正相关,而AOSZ的前额叶和皮层下结构与神经正向正相关。因此,C4A和C4B GCN在经常与精神分裂症有关的区域与神经纤维收缩有关,并且可能在神经成熟上具有依赖性。

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