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与小鼠成熟和衰老相关的脑结构及工作记忆适应性

Brain structure and working memory adaptations associated with maturation and aging in mice.

作者信息

Clifford Kevan P, Miles Amy E, Prevot Thomas D, Misquitta Keith A, Ellegood Jacob, Lerch Jason P, Sibille Etienne, Nikolova Yuliya S, Banasr Mounira

机构信息

Institute of Medical Sciences, University of Toronto, Toronto, ON, Canada.

Centre for Addiction and Mental Health, Toronto, ON, Canada.

出版信息

Front Aging Neurosci. 2023 Jul 6;15:1195748. doi: 10.3389/fnagi.2023.1195748. eCollection 2023.

Abstract

INTRODUCTION

As the population skews toward older age, elucidating mechanisms underlying human brain aging becomes imperative. Structural MRI has facilitated non-invasive investigation of lifespan brain morphology changes, yet this domain remains uncharacterized in rodents despite increasing use as models of disordered human brain aging.

METHODS

Young (2m, = 10), middle-age (10m, = 10) and old (22m, = 9) mice were utilized for maturational (young vs. middle-age) and aging-related (middle-age vs. old mice) comparisons. Regional brain volume was averaged across hemispheres and reduced to 32 brain regions. Pairwise group differences in regional volume were tested using general linear models, with total brain volume as a covariate. Sample-wide associations between regional brain volume and Y-maze performance were assessed using logistic regression, residualized for total brain volume. Both analyses corrected for multiple comparisons. Structural covariance networks were generated using the R package "igraph." Group differences in network centrality (degree), integration (mean distance), and segregation (transitivity, modularity) were tested across network densities (5-40%), using 5,000 (1,000 for degree) permutations with significance criteria of < 0.05 at ≥5 consecutive density thresholds.

RESULTS

Widespread significant maturational changes in volume occurred in 18 brain regions, including considerable loss in isocortex regions and increases in brainstem regions and white matter tracts. The aging-related comparison yielded 6 significant changes in brain volume, including further loss in isocortex regions and increases in white matter tracts. No significant volume changes were observed across either comparison for subcortical regions. Additionally, smaller volume of the anterior cingulate area (χ = 2.325, = 0.044) and larger volume of the hippocampal formation (χ = -2.180, = 0.044) were associated with poorer cognitive performance. Maturational network comparisons yielded significant degree changes in 9 regions, but no aging-related changes, aligning with network stabilization trends in humans. Maturational decline in modularity occurred (24-29% density), mirroring human trends of decreased segregation in young adulthood, while mean distance and transitivity remained stable.

CONCLUSION/IMPLICATIONS: These findings offer a foundational account of age effects on brain volume, structural brain networks, and working memory in mice, informing future work in facilitating translation between rodent models and human brain aging.

摘要

引言

随着人口趋向老龄化,阐明人类大脑衰老的潜在机制变得势在必行。结构磁共振成像(MRI)有助于对大脑寿命期形态变化进行无创性研究,然而,尽管啮齿动物作为人类大脑衰老紊乱模型的应用日益广泛,但该领域在啮齿动物中仍未得到充分研究。

方法

使用年轻(2个月,n = 10)、中年(10个月,n = 10)和老年(22个月,n = 9)小鼠进行成熟相关(年轻与中年)和衰老相关(中年与老年小鼠)的比较。将大脑区域体积在半球间进行平均,并缩减为32个脑区。使用一般线性模型测试区域体积的成对组间差异,并将全脑体积作为协变量。使用逻辑回归评估全样本范围内脑区体积与Y迷宫表现之间的关联,并对全脑体积进行残差分析。两种分析均对多重比较进行了校正。使用R包“igraph”生成结构协方差网络。在网络密度(5 - 40%)范围内,使用5000次(度分析为1000次)排列检验网络中心性(度)、整合性(平均距离)和分离性(传递性、模块性)的组间差异,显著性标准为在≥5个连续密度阈值下p < 0.05。

结果

18个脑区出现了广泛的显著成熟变化,包括等皮质区域的显著减少以及脑干区域和白质束的增加。衰老相关比较产生了6个脑区体积的显著变化,包括等皮质区域的进一步减少和白质束的增加。在这两种比较中,皮质下区域均未观察到显著的体积变化。此外,前扣带区体积较小(χ = 2.325,p = 0.044)和海马结构体积较大(χ = -2.180,p = 0.044)与较差的认知表现相关。成熟网络比较在9个区域产生了显著的度变化,但未发现与衰老相关的变化,这与人类的网络稳定趋势一致。在24 - 29%密度下出现了模块性的成熟下降,反映了人类成年早期分离性降低的趋势,而平均距离和传递性保持稳定。

结论/启示:这些发现为年龄对小鼠脑体积、脑结构网络和工作记忆的影响提供了基础描述,为促进啮齿动物模型与人类大脑衰老之间的转化研究提供了参考。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/010c/10359104/01b6528b2061/fnagi-15-1195748-g001.jpg

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