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White matter alterations in antipsychotic- and mood stabilizer-naïve individuals with bipolar II/NOS disorder

机译:患有抗精神病药和无情绪稳定剂的双相性II / NOS疾病患者的白质变化

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摘要

Structural magnetic resonance imaging (MRI) studies using voxel-based morphometry (VBM) and tract-based spatial statistics (TBSS) have been inconsistent in demonstrating impairments in gray matter (GM) and white matter (WM) structures in bipolar disorder (BD). This may be a consequence of significant confounding effects of medication, illness history and selection of controls in existing studies. Study of bipolar II or not-otherwise-specified (BD II/NOS) disorder provides a solution to these confounds and a bridge to unipolar cases across the affective spectrum.Thirty-eight euthymic, antipsychotic- and mood stabilizer-naïve young adults (mean age = 20.9 years) with BD II/NOS and 37 age-, cognitive ability- and gender-matched healthy controls (HCs) underwent MRI. Voxel-wise and regional gray matter volume comparisons were conducted using voxel-based morphometry (VBM). Tract-based spatial statistics (TBSS) were used to assess whole-brain WM, as indexed using fractional anisotropy (FA), mean diffusivity (MD), parallel and perpendicular diffusion values. No between-group differences were observed for whole-brain VBM comparisons. By contrast, in comparison to HCs, participants with BD II/NOS had significant widespread reductions in FA and increased MD and perpendicular diffusion values in virtually all the major cortical white matter tracts.These data suggest pathophysiological involvement of WM microstructures – but not GM macrostructures – in high functioning BD II/NOS patients at an early age and before significant clinical adversity has been recorded. We propose that white matter development is a valid candidate target for understanding genetic and environmental antecedents to bipolar disorder and mood disorder more generally.
机译:使用基于体素的形态计量学(VBM)和基于道的空间统计学(TBSS)的结构磁共振成像(MRI)研究在证明双相情感障碍(BD)中的灰质(GM)和白质(WM)结构受损方面一直不一致。这可能是药物,疾病史和现有研究中对照选择的显着混淆影响的结果。对双相性II型或其他非特定性(BD II / NOS)障碍的研究提供了解决这些混淆的方法,并为跨情感谱的单相性病例提供了桥梁.38名幼稚,有抗精神病药和情绪稳定剂的年轻成年人(平均BD II / NOS年龄= 20.9岁)和37位年龄,认知能力和性别匹配的健康对照(HCs)接受了MRI检查。使用基于体素的形态计量学(VBM)进行体素方向和区域灰质体积比较。基于分数的空间统计(TBSS)用于评估全脑WM,使用分数各向异性(FA),平均扩散率(MD),平行和垂直扩散值进行索引。对于全脑VBM比较,未观察到组间差异。相比之下,与HCs相比,BD II / NOS参与者几乎在所有主要的皮质白质区中均具有广泛的FA降低,MD和垂直扩散值显着升高。这些数据表明WM微观结构的病理生理参与-但GM宏观结构没有–早年且未记录严重临床逆境的高功能BD II / NOS患者。我们提出白质发育是更广泛地理解双相情感障碍和情绪障碍的遗传和环境先兆的有效候选对象。

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