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探究重复性头部撞击暴露与慢性创伤性脑病的血浆蛋白质组。

Interrogating the plasma proteome of repetitive head impact exposure and chronic traumatic encephalopathy.

作者信息

Saloner Rowan, Casaletto Kaitlin B, Rayaprolu Sruti, Cornelis Louisa, Chakrabarty Paramita, Abisambra Jose F, Spina Salvatore, Grinberg Lea T, Seeley William W, Miller Bruce L, Kramer Joel H, Rabinovici Gil D, Asken Breton M

机构信息

Department of Neurology, Memory and Aging Center, University of California, San Francisco, 675 Nelson Rising Lane, San Francisco, CA, USA.

Department of Neuroscience, Center for Translational Research in Neurodegenerative Disease, University of Florida, 1275 Center Drive, Gainesville, FL, USA.

出版信息

Mol Neurodegener. 2025 Jun 16;20(1):71. doi: 10.1186/s13024-025-00860-x.

Abstract

BACKGROUND

Exposure to repetitive head impacts (RHI) is associated with increased risk for chronic traumatic encephalopathy (CTE), a neurodegenerative tauopathy, and other neuropathological changes. Biological drivers of RHI-related neurodegeneration are not well understood. We interrogated the plasma proteome in aging adults with prior RHI compared to healthy controls (CTL) and individuals with Alzheimer's disease (AD), including a subset characterized neuropathologically at autopsy.

METHODS

Proximity extension assay (Olink Explore®) quantified 2,779 plasma proteins in 22 RHI patients (all AD-biomarker negative), 39 biomarker-confirmed AD, and 44 CTL. A subset of participants went to autopsy (N = 16) allowing for comparisons of the antemortem plasma proteome between autopsy-confirmed CTE + (N = 7) and CTE- (N = 9). Differential abundance and co-expression network analyses identified plasma proteomic signatures of RHI, which were functionally annotated using gene ontology and cell type enrichment analysis. Nonparametric correlations examined plasma proteomic associations with orthogonally-measured plasma biomarkers, global cognitive function, and semi-quantitative ratings of neuropathology burden at autopsy.

RESULTS

Differential abundance analysis revealed 434 increased (vs. 6 decreased) proteins in RHI vs. CTL and 193 increased (vs. 14 decreased) in RHI vs. AD. Network analysis identified 9 protein co-expression modules (M1-M9), of which 7 were elevated in RHI compared to AD or CTL. Modules with increased abundance in RHI were enriched for mitochondrial/metabolic, cell division, and immunovascular (e.g., cell adhesion, TNF-signaling) processes. RHI-related modules exhibited strong and selective correlations with immunoassay-based plasma IL-6 in RHI cases, including the M2 TNF-signaling/cell adhesion module which harbored proteins that strongly tracked with cognitive function. RHI-related plasma protein signatures were similar in the subset of participants with autopsy-confirmed CTE, including immune and metabolic modules that positively correlated with medial temporal lobe tau and TDP-43 burden.

CONCLUSIONS

Molecular pathways in plasma most consistently implicated in RHI were tied to immune response, mitochondrial function, and cell metabolism. RHI-related proteomic signatures tracked with antemortem cognitive severity and postmortem neuropathological burden, providing converging evidence for their role in disease progression. Differentially abundant proteins and co-expression modules in RHI may inform mechanisms linking RHI to increased dementia risk, thus guiding diagnostic biomarker and therapeutic development for at-risk populations.

摘要

背景

反复头部撞击(RHI)与慢性创伤性脑病(CTE,一种神经退行性tau蛋白病)及其他神经病理学改变的风险增加相关。RHI相关神经退行性变的生物学驱动因素尚不清楚。我们对有RHI史的老年人与健康对照(CTL)以及阿尔茨海默病(AD)患者的血浆蛋白质组进行了研究,其中包括一组经尸检进行神经病理学特征分析的亚组。

方法

邻近延伸分析(Olink Explore®)对22例RHI患者(均为AD生物标志物阴性)、39例经生物标志物确诊的AD患者和44例CTL中的2779种血浆蛋白进行了定量分析。一部分参与者进行了尸检(N = 16),以便比较尸检确诊的CTE阳性(N = 7)和CTE阴性(N = 9)患者生前的血浆蛋白质组。差异丰度分析和共表达网络分析确定了RHI的血浆蛋白质组特征,并使用基因本体论和细胞类型富集分析对其进行了功能注释。非参数相关性分析检测了血浆蛋白质组与正交测量的血浆生物标志物、整体认知功能以及尸检时神经病理学负担的半定量评分之间的关联。

结果

差异丰度分析显示,与CTL相比,RHI患者中有434种蛋白质增加(6种减少),与AD相比,RHI患者中有193种蛋白质增加(14种减少)。网络分析确定了9个蛋白质共表达模块(M1 - M9),其中7个在RHI患者中相对于AD或CTL升高。RHI中丰度增加的模块富含线粒体/代谢、细胞分裂和免疫血管(如细胞粘附、TNF信号传导)过程。在RHI病例中,与RHI相关的模块与基于免疫测定法的血浆IL-6呈现出强烈且选择性的相关性,包括M2 TNF信号传导/细胞粘附模块,该模块中的蛋白质与认知功能密切相关。在经尸检确诊为CTE的参与者亚组中,与RHI相关的血浆蛋白质特征相似,包括与内侧颞叶tau蛋白和TDP - 43负担呈正相关的免疫和代谢模块。

结论

血浆中最常与RHI相关的分子途径与免疫反应、线粒体功能和细胞代谢有关。与RHI相关的蛋白质组特征与生前认知严重程度和死后神经病理学负担相关,为它们在疾病进展中的作用提供了一致的证据。RHI中差异丰度的蛋白质和共表达模块可能为将RHI与痴呆风险增加联系起来的机制提供信息,从而指导针对高危人群的诊断生物标志物和治疗方法的开发。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d88b/12168330/b5407526e5d1/13024_2025_860_Fig1_HTML.jpg

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