Hippocampal GFAP-positive astrocyte responses to amyloid and tau pathologies

海马结构 星形胶质细胞 胶质纤维酸性蛋白 星形胶质增生 神经科学 生物 背景(考古学) 转录组 阿尔茨海默病 医学 病理 基因表达 免疫学 基因 疾病 遗传学 免疫组织化学 中枢神经系统 古生物学
作者
Marco Antônio De Bastiani,Bruna Bellaver,Wagner S. Brum,Débora Guerini de Souza,Pâmela C.L. Ferreira,Andréia Silva da Rocha,Guilherme Povala,João Pedro Ferrari‐Souza,Andréa Lessa Benedet,Nicholas J. Ashton,Thomas K. Karikari,Henrik Zetterberg,Kaj Blennow,Pedro Rosa‐Neto,Tharick A. Pascoal,Eduardo R. Zimmer
出处
期刊:Brain Behavior and Immunity [Elsevier]
卷期号:110: 175-184 被引量:24
标识
DOI:10.1016/j.bbi.2023.03.001
摘要

In Alzheimer’s disease clinical research, glial fibrillary acidic protein (GFAP) released/leaked into the cerebrospinal fluid and blood is widely measured and perceived as a biomarker of reactive astrogliosis. However, it was demonstrated that GFAP levels differ in individuals presenting with amyloid-β (Aβ) or tau pathologies. The molecular underpinnings behind this specificity are little explored. Here we investigated biomarker and transcriptomic associations of hippocampal GFAP-positive astrocytes with Aβ and tau pathologies in humans and mouse models. We studied 90 individuals with plasma GFAP, Aβ- and Tau-PET to investigate the association between biomarkers. Then, transcriptomic analysis in hippocampal GFAP-positive astrocytes isolated from mouse models presenting Aβ (PS2APP) or tau (P301S) pathologies was conducted to explore differentially expressed genes (DEGs), Gene Ontology terms, and protein–protein interaction networks associated with each phenotype. In humans, we found that plasma GFAP associates with Aβ but not tau pathology. Unveiling the unique nature of hippocampal GFAP-positive astrocytic responses to Aβ or tau pathologies, mouse transcriptomics showed scarce overlap of DEGs between the Aβ. and tau mouse models. While Aβ GFAP-positive astrocytes were overrepresented with DEGs associated with proteostasis and exocytosis-related processes, tau hippocampal GFAP-positive astrocytes presented greater abnormalities in functions related to DNA/RNA processing and cytoskeleton dynamics. Our results offer insights into Aβ- and tau-driven specific signatures in hippocampal GFAP-positive astrocytes. Characterizing how different underlying pathologies distinctly influence astrocyte responses is critical for the biological interpretation of astrocyte biomarkers and suggests the need to develop context-specific astrocyte targets to study AD. This study was supported by Instituto Serrapilheira, Alzheimer’s Association, CAPES, CNPq and FAPERGS.
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