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睡眠质量差者的髓鞘变化:对类淋巴系统清除功能和区域生物钟基因表达的见解

Myelin Changes in Poor Sleepers: Insights into Glymphatic Clearance Function and Regional Circadian Clock Gene Expression.

作者信息

Andica Christina, Kamagata Koji, Takabayashi Kaito, Mahemuti Zaimire, Iwasaki Manabu, Hagiwara Akifumi, Uchida Wataru, Tabata Hiroki, Naito Hitoshi, Kaga Hideyoshi, Someya Yuki, Tamura Yoshifumi, Kawamori Ryuzo, Watada Hirotaka, Aoki Shigeki

机构信息

Department of Radiology, Juntendo University Graduate School of Medicine, Tokyo, Japan.

Faculty of Health Data Science, Juntendo University, Chiba, Japan.

出版信息

Aging Dis. 2024 Aug 13;16(4):2453-2467. doi: 10.14336/AD.2024.0894.

Abstract

Sleep is essential for maintaining brain myelin integrity. Emerging evidence suggests that poor sleep quality compromises the glymphatic system, a perivascular network crucial for brain waste clearance, leading to the accumulation of neuroinflammatory and toxic proteins, which may affect myelin integrity. Furthermore, poor sleep quality results in alterations in gene expression within the brain. We evaluated the associations among poor sleep quality, brain myelin integrity, and glymphatic clearance function as well as the impact of circadian clock gene expression on regional cortical myelin content. 50 poor sleepers (average age 71.08 ± 4.69 years; Pittsburgh Sleep Quality Index [PSQI] > 5) and 50 good sleepers (average age 73.04 ± 5.80 years; PSQI ≤ 5) were assessed. Myelin volume fraction (MVF) was quantified using magnetization transfer saturation imaging, and glymphatic function was noninvasively examined using diffusion tensor imaging along the perivascular space. Circadian gene expression was analyzed using postmortem brain tissue from the Allen Human Brain Atlas. Magnetic resonance imaging measures were correlated with cognitive and depression scores. Lower MVF was observed in the fronto-temporo-parietal and limbic regions as well as in major white matter tracts in poor sleepers compared with that in good sleepers. This reduction was linked to lower cognitive function scores and higher depressive scores. Poor sleepers also exhibited lower diffusivity along the perivascular spaces, mediating the relationship between poor sleep quality and demyelination. Regions with higher expression of CLOCK, CRY2, PER1, and PER2 exhibited greater MVF disparities between good and poor sleepers, whereas lower expression of CRY1 was associated with more pronounced differences. Poor sleep quality was associated with lower brain myelin integrity, correlating with reduced cognitive performance and increased depressive symptoms. These changes might be mediated by glymphatic clearance dysfunction and were associated with the differential expression of circadian clock genes.

摘要

睡眠对于维持大脑髓鞘完整性至关重要。新出现的证据表明,睡眠质量差会损害类淋巴系统,这是一个对大脑废物清除至关重要的血管周围网络,导致神经炎症和毒性蛋白的积累,这可能会影响髓鞘完整性。此外,睡眠质量差会导致大脑内基因表达的改变。我们评估了睡眠质量差、大脑髓鞘完整性和类淋巴清除功能之间的关联,以及昼夜节律时钟基因表达对区域皮质髓鞘含量的影响。评估了50名睡眠质量差的人(平均年龄71.08±4.69岁;匹兹堡睡眠质量指数[PSQI]>5)和50名睡眠质量好的人(平均年龄73.04±5.80岁;PSQI≤5)。使用磁化传递饱和成像对髓鞘体积分数(MVF)进行定量,并使用沿血管周围间隙的扩散张量成像对类淋巴功能进行无创检查。使用来自艾伦人类大脑图谱的死后脑组织分析昼夜节律基因表达。磁共振成像测量结果与认知和抑郁评分相关。与睡眠质量好的人相比,睡眠质量差的人在额颞顶叶和边缘区域以及主要白质束中观察到较低的MVF。这种降低与较低的认知功能评分和较高的抑郁评分有关。睡眠质量差的人在血管周围间隙也表现出较低的扩散率,介导了睡眠质量差与脱髓鞘之间的关系。CLOCK、CRY2、PER1和PER2表达较高的区域在睡眠质量好和差的人之间表现出更大的MVF差异,而CRY1表达较低与更明显的差异相关。睡眠质量差与较低的大脑髓鞘完整性相关,与认知能力下降和抑郁症状增加相关。这些变化可能由类淋巴清除功能障碍介导,并与昼夜节律时钟基因的差异表达有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c632/12221392/c35a49315548/AD-16-4-2453-g1.jpg

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