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淀粉样体与阿尔茨海默病中的海马体tau病理呈负相关。

Corpora amylacea negatively correlate with hippocampal tau pathology in Alzheimer's disease.

作者信息

Dallmeier Julian D, Gober Ryan, Vontell Regina T, Barreda Ayled, Dorfsman Daniel A, Davis David A, Sun Xiaoyan, Brzostowicki Daniel, Bennett Illiana, Garamszegi Susanna P, Wander Connor M, Cohen Todd, Scott William K

机构信息

Brain Endowment Bank, Department of Neurology, University of Miami Miller School of Medicine, Miami, FL, United States.

Department of Neurology, Evelyn F. McKnight Brain Institute, University of Miami Miller School of Medicine, Miami, FL, United States.

出版信息

Front Neurosci. 2024 Feb 29;18:1286924. doi: 10.3389/fnins.2024.1286924. eCollection 2024.

Abstract

INTRODUCTION

Severity and distribution of aggregated tau and neurofibrillary tangles (NFT) are strongly correlated with the clinical presentation of Alzheimer's disease (AD). Clearance of aggregated tau could decrease the rate of NFT formation and delay AD onset. Recent studies implicate corpora amylacea (CA) as a regulator of onset or accumulation of tau pathology. Normally, CA clear brain waste products by amassing cellular debris, which are then extruded into the cerebrospinal fluid to be phagocytosed. The proper functioning of CA may slow progression of AD-associated NFT pathology, and this relationship may be influenced by amount and distribution of phospho-tau (pTau) produced, age, sex, and genetic risk.

OBJECTIVE

The goal of this study was to determine if CA size and number are associated with hippocampal location and local pTau severity while accounting for variations in age, sex, and genetic risk.

METHODS

Postmortem brain hippocampal tissue sections from 40 AD and 38 unaffected donors were immunohistochemically stained with AT8 (pTau) and counter stained with periodic acid Schiff (PAS). Stained sections of the CA1 and CA3 regions of the hippocampus were analyzed. The percent area occupied (%AO) of CA, pTau, and NFT was calculated. Pairwise comparisons and regression modeling were used to analyze the influence of age, pTau %AO, and genetic risk on %AO by CA in each region, separately in donors with AD and unaffected donors.

RESULTS

CA %AO was significantly higher in the CA3 region compared to CA1 in both groups. A significant negative correlation of CA %AO with both pTau %AO and neurofibrillary tangle %AO in the CA3 region of AD brain donors was found. Regression analysis in the CA3 region revealed a significant negative association between CA with both pTau and age.

CONCLUSION

We found an increase of CA in the CA3 region, compared to CA1 region, in AD and unaffected donors. This may suggest that the CA3 region is a hub for waste removal. Additionally, the negative correlation between %AO by CA and NFT in the CA3 region of the hippocampus in donors with AD suggests CA could play a role in AD pathologic progression by influencing tau clearance.

摘要

引言

聚集的tau蛋白和神经原纤维缠结(NFT)的严重程度及分布与阿尔茨海默病(AD)的临床表现密切相关。清除聚集的tau蛋白可降低NFT的形成速率并延缓AD的发病。最近的研究表明淀粉样体(CA)是tau病理发生或积累的调节因子。正常情况下,CA通过积累细胞碎片来清除脑内废物,这些碎片随后被挤出到脑脊液中被吞噬。CA的正常功能可能会减缓AD相关NFT病理的进展,这种关系可能会受到所产生的磷酸化tau(pTau)的量和分布、年龄、性别及遗传风险的影响。

目的

本研究的目的是在考虑年龄、性别和遗传风险差异的情况下,确定CA的大小和数量是否与海马位置及局部pTau严重程度相关。

方法

对40例AD患者和38例未受影响供体的死后脑海马组织切片进行免疫组织化学染色,用AT8(pTau)染色,并用过碘酸希夫(PAS)复染。对海马CA1和CA3区域的染色切片进行分析。计算CA、pTau和NFT所占的面积百分比(%AO)。采用成对比较和回归模型分别分析AD患者和未受影响供体中年龄、pTau %AO和遗传风险对各区域CA %AO的影响。

结果

两组中CA3区域的CA %AO均显著高于CA1区域。在AD脑供体的CA3区域,发现CA %AO与pTau %AO和神经原纤维缠结%AO均呈显著负相关。CA3区域的回归分析显示CA与pTau和年龄均呈显著负相关。

结论

我们发现,与CA1区域相比,AD患者和未受影响供体的CA3区域中CA增加。这可能表明CA3区域是废物清除的中心。此外,AD供体海马CA3区域中CA %AO与NFT之间的负相关表明,CA可能通过影响tau清除在AD病理进展中发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6441/10937356/1c14ee011bfa/fnins-18-1286924-g001.jpg

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