Palmitic Acid Upregulates Type I Interferon–Mediated Antiviral Response and Cholesterol Biosynthesis in Human Astrocytes

被引:0
|
作者
Alexis Felipe Rojas-Cruz
Cynthia Alexandra Martín-Jiménez
Janneth González
Yeimy González-Giraldo
Andrés Mauricio Pinzón
George E. Barreto
Andrés Felipe Aristizábal-Pachón
机构
[1] Pontificia Universidad Javeriana,Departamento de Nutrición Y Bioquímica, Facultad de Ciencias
[2] Medical College of Georgia at Augusta University,Department of Neuroscience and Regenerative Medicine
[3] Universidad Nacional de Colombia,Laboratorio de Bioinformática Y Biología de Sistemas
[4] University of Limerick,Department of Biological Sciences
来源
Molecular Neurobiology | 2023年 / 60卷
关键词
Human astrocytes; Lipotoxicity; Tibolone; RNA-seq; Neuroinflammation; Lipid metabolism;
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学科分类号
摘要
Chronic intake of a high-fat diet increases saturated fatty acids in the brain causing the progression of neurodegenerative diseases. Palmitic acid is a free fatty acid abundant in the diet that at high concentrations may penetrate the blood–brain barrier and stimulate the production of pro-inflammatory cytokines, leading to inflammation in astrocytes. The use of the synthetic neurosteroid tibolone in protection against fatty acid toxicity is emerging, but its transcriptional effects on palmitic acid–induced lipotoxicity remain unclear. Herein, we performed a transcriptome profiling of normal human astrocytes to investigate the molecular mechanisms by which palmitic acid causes cellular damage to astrocytes, and whether tibolone could reverse its detrimental effects. Astrocytes undergo a profound transcriptional change at 2 mM palmitic acid, affecting the expression of 739 genes, 366 upregulated and 373 downregulated. However, tibolone at 10 nM does not entirely reverse palmitic acid effects. Additionally, the protein–protein interaction reveals two novel gene clustering modules. The first module involves astrocyte defense responses by upregulation of pathways associated with antiviral innate immunity, and the second is linked to lipid metabolism. Our data suggest that activation of viral response signaling pathways might be so far, the initial molecular mechanism of astrocytes in response to a lipotoxic insult by palmitic acid, triggered particularly upon increased expression levels of IFIT2, IRF1, and XAF1. Therefore, this novel approach using a global gene expression analysis may shed light on the pleiotropic effects of palmitic acid on astrocytes, and provide a basis for future studies addressed to elucidate these responses in neurodegenerative conditions, which is highly valuable for the design of therapeutic strategies.
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页码:4842 / 4854
页数:12
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