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No effect of 5HTTLPR or BDNF Val66Met polymorphism on hippocampal morphology in major depression

机译:5HTTLpR或BDNF Val66met多态性对抑郁症大鼠海马形态无影响

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摘要

Neuroimaging research implicates the hippocampus in the aetiology of major depressive disorder (MDD). Imaging genetics studies have investigated the influence of the serotonin transporter-linked polymorphic region (5HTTLPR) and brain-derived neurotrophic factor (BDNF) Val66Met polymorphism on the hippocampus in healthy individuals and patients with depression (MDD). However, conflicting results have led to inconclusive evidence about the effect of 5HTTLPR or BDNF on hippocampal volume (HCV). We hypothesized that analysis methods based on three-dimensional (3D) hippocampal shape mapping could offer improved sensitivity to clarify these effects. Magnetic resonance imaging data were collected in parallel samples of 111 healthy individuals and 84 MDD patients. Manual hippocampal segmentation was conducted and the resulting data used to investigate the influence of 5HTTLPR and BDNF Val66Met genotypes on HCV and 3D shape within each sample. Hippocampal volume normalized by intracranial volume (ICV) showed no significant difference between 5HTTLPR S allele carriers and L/L homozygotes or between BDNF Met allele carriers and Val/Val homozygotes in the group of healthy individuals. Moreover, there was no significant difference in normalized HCV between 5HTTLPR diallelic and triallelic classifications or between the BDNF Val66Met genotypes in MDD patients, although there was a relationship between BDNF Val66Met and ICV. Shape analysis detected dispersed between-group differences, but these effects did not survive multiple testing correction. In this study, there was no evidence of a genetic effect for 5HTTLPR or BDNF Val66Met on hippocampal morphology in either healthy individuals or MDD patients despite the relatively large sample sizes and sensitive methodology.
机译:神经影像学研究将海马体牵涉到重度抑郁症(MDD)的病因中。影像遗传学研究已经研究了5-羟色胺转运蛋白相关多态性区域(5HTTLPR)和脑源性神经营养因子(BDNF)Val66Met多态性对健康人和抑郁症患者(MDD)海马的影响。但是,矛盾的结果导致了关于5HTTLPR或BDNF对海马体积(HCV)的影响的不确定性证据。我们假设基于三维(3D)海马形状映射的分析方法可以提供更高的灵敏度来阐明这些影响。在111名健康个体和84名MDD患者的平行样本中收集了磁共振成像数据。进行了手动海马分割,所得数据用于研究5HTTLPR和BDNF Val66Met基因型对每个样品中HCV和3D形状的影响。在健康个体组中,以颅内体积(ICV)标准化的海马体积显示5HTTLPR S等位基因携带者与L / L纯合子之间或BDNF Met等位基因携带者与Val / Val纯合子之间无显着差异。此外,尽管BDNF Val66Met与ICV之间存在相关性,但5HTTLPR透析和三叶分类之间或BDNF Val66Met基因型之间的标准化HCV没有显着差异。形状分析检测到分散的组间差异,但这些效果在多次测试校正后均无法幸免。在这项研究中,尽管样本量和敏感性较高,但没有证据表明5HTTLPR或BDNF Val66Met对健康个体或MDD患者的海马形态有遗传影响。

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