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早产儿出生后长达 13 年的脑白质纤维密度和形态的长期发育:基于固定点分析。

Long-term development of white matter fibre density and morphology up to 13 years after preterm birth: A fixel-based analysis.

机构信息

Victorian Infant Brain Study (VIBeS), Murdoch Children's Research Institute, Melbourne, Australia; Developmental Imaging, Murdoch Children's Research Institute, Melbourne, Australia.

Victorian Infant Brain Study (VIBeS), Murdoch Children's Research Institute, Melbourne, Australia; Developmental Imaging, Murdoch Children's Research Institute, Melbourne, Australia; Department of Paediatrics, The University of Melbourne, Melbourne, Australia; Florey Institute of Neuroscience and Mental Health, Melbourne, Australia.

出版信息

Neuroimage. 2020 Oct 15;220:117068. doi: 10.1016/j.neuroimage.2020.117068. Epub 2020 Jun 22.

Abstract

BACKGROUND

It is well documented that infants born very preterm (VP) are at risk of brain injury and altered brain development in the neonatal period, however there is a lack of long-term, longitudinal studies on the effects of VP birth on white matter development over childhood. Most previous studies were based on voxel-averaged, non-fibre-specific diffusion magnetic resonance imaging (MRI) measures, such as fractional anisotropy. In contrast, the novel diffusion MRI analysis framework, fixel-based analysis (FBA), enables whole-brain analysis of microstructural and macrostructural properties of individual fibre populations at a sub-voxel level. We applied FBA to investigate the long-term implications of VP birth and associated perinatal risk factors on fibre development in childhood and adolescence.

METHODS

Diffusion images were acquired for a cohort of VP (born <30 weeks' gestation) and full-term (FT, ≥37 weeks' gestation) children at two timepoints: mean (SD) 7.6 (0.2) years (n ​= ​138 VP and 32 FT children) and 13.3 (0.4) years (n ​= ​130 VP and 45 FT children). 103 VP and 21 FT children had images at both ages for longitudinal analysis. At every fixel (individual fibre population within an image voxel) across the white matter, we compared FBA metrics (fibre density (FD), cross-section (FC) and a combination of these properties (FDC)) between VP and FT groups cross-sectionally at each timepoint, and longitudinally between timepoints. We also examined associations between known perinatal risk factors and FBA metrics in the VP group.

RESULTS

Compared with FT children, VP children had lower FD, FC and FDC throughout the white matter, particularly in the corpus callosum, tapetum, inferior fronto-occipital fasciculus, fornix and cingulum at ages 7 and 13 years, as well as the corticospinal tract and anterior limb of the internal capsule at age 13 years. VP children also had slower FDC development in the corpus callosum and corticospinal tract between ages 7 and 13 years compared with FT children. Within VP children, earlier gestational age at birth, lower birth weight z-score, and neonatal brain abnormalities were associated with lower FD, FC and FDC throughout the white matter at both ages.

CONCLUSIONS

VP birth and concomitant perinatal risk factors are associated with fibre tract-specific alterations to axonal development in childhood and adolescence.

摘要

背景

已有大量文献证明,极早早产(VP)婴儿在新生儿期存在脑损伤和脑发育改变的风险,然而,关于 VP 出生对儿童期白质发育影响的长期、纵向研究却很少。大多数先前的研究都是基于体素平均的、非纤维特异性的扩散磁共振成像(MRI)测量,如各向异性分数。相比之下,新型扩散 MRI 分析框架——纤维束固定分析(FBA),可以在亚像素水平上对个体纤维束群的微观和宏观结构特性进行全脑分析。我们应用 FBA 研究了 VP 出生及相关围产期危险因素对儿童和青少年时期纤维发育的长期影响。

方法

我们对一组 VP(<30 周妊娠)和 FT(≥37 周妊娠)儿童进行了两次扩散成像采集:平均(标准差)7.6(0.2)岁(n=138 名 VP 和 32 名 FT 儿童)和 13.3(0.4)岁(n=130 名 VP 和 45 名 FT 儿童)。103 名 VP 和 21 名 FT 儿童在两个年龄段均有图像,用于纵向分析。在每个白质的每个纤维束(图像体素内的单个纤维束群)中,我们比较了 VP 和 FT 组在每个时间点的 FBA 指标(纤维密度(FD)、纤维交叉(FC)和这些特性的组合(FDC)),以及在时间点之间的纵向比较。我们还在 VP 组中研究了已知围产期危险因素与 FBA 指标之间的关联。

结果

与 FT 儿童相比,VP 儿童在 7 岁和 13 岁时整个白质,特别是胼胝体、视丘、下额枕束、穹窿和扣带回,以及 13 岁时皮质脊髓束和内囊前肢的 FD、FC 和 FDC 均较低。与 FT 儿童相比,VP 儿童在 7 岁至 13 岁期间,胼胝体和皮质脊髓束的 FDC 发育速度也较慢。在 VP 儿童中,出生时胎龄更早、出生体重 z 评分更低以及新生儿脑异常与整个白质的 FD、FC 和 FDC 均较低有关。

结论

VP 出生和伴随的围产期危险因素与儿童和青少年时期轴突发育的纤维束特异性改变有关。

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