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精神分裂症相关神经调节蛋白 1 单核苷酸多态性导致大样本青年男性平滑眼追踪缺陷。

Schizophrenia-related neuregulin-1 single-nucleotide polymorphisms lead to deficient smooth eye pursuit in a large sample of young men.

机构信息

Psychiatry Department, National and Kapodistrian University of Athens Medical School, Eginition Hospital, 72 Vas. Sofias Avenue, Athens, Greece.

出版信息

Schizophr Bull. 2011 Jul;37(4):822-31. doi: 10.1093/schbul/sbp150. Epub 2009 Dec 4.

Abstract

Neuregulin-1 (NRG1) variations have been shown to modulate schizophrenia candidate endophenotypes related to brain structure and function. The aim of this study was to determine the effect of NRG1 on several oculomotor schizophrenia endophenotypes. The effects of 5 core single-nucleotide polymorphisms (SNPs) within the NRG1 gene to oculomotor parameters in a battery of oculomotor tasks (saccade, antisaccade, smooth eye pursuit, fixation) were investigated in a sample of 2243 young male military conscripts. Additive regression models, bootstrap and permutation techniques, were used as well as structural equation modeling and haplotype analysis. A deficit in global smooth eye pursuit performance measured using the root-mean-square error (RMSE) was related to the risk allele of SNP8NRG243177, and a deficit in global smooth eye pursuit performance measured using the saccade frequency was related with the risk allele of SNP8NRG433E1006. Structural equation modeling confirmed a global effect of NRG1 genotype on smooth eye pursuit performance using the RMSE, while the effect on saccade frequency was not confirmed. Haplotype analysis further confirmed the prediction from the structural equation modeling that a combination of alleles corresponding to the Icelandic high-risk haplotype was related to a deficit in global pursuit performance. NRG1 genotype variations were related to smooth eye pursuit variations both at the SNP level and at the haplotype level adding to the validation of this gene as a candidate gene for the disorder.

摘要

神经调节蛋白 1(NRG1)的变异已被证明可调节与大脑结构和功能相关的精神分裂症候选内表型。本研究旨在确定 NRG1 对几种眼动精神分裂症内表型的影响。在一项眼动任务(扫视、反扫视、平滑眼追踪、固视)的眼动参数电池中,研究了 NRG1 基因内的 5 个核心单核苷酸多态性(SNP)对眼动参数的影响,该研究样本包括 2243 名年轻男性新兵。使用加性回归模型、引导和置换技术以及结构方程模型和单体型分析来研究 SNP8NRG243177 的风险等位基因与使用均方根误差(RMSE)测量的整体平滑眼追踪性能缺陷之间的关系,以及 SNP8NRG433E1006 的风险等位基因与使用扫视频率测量的整体平滑眼追踪性能缺陷之间的关系。结构方程模型证实了 NRG1 基因型对使用 RMSE 的平滑眼追踪性能的整体影响,而对扫视频率的影响则未得到证实。单体型分析进一步证实了结构方程建模的预测,即与冰岛高危单体型相对应的等位基因组合与整体追踪表现缺陷有关。NRG1 基因型变异与平滑眼追踪变异有关,无论是在 SNP 水平还是单体型水平,这都增加了该基因作为该疾病候选基因的验证。

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