4.6 Article

Hypercholesterolemia and 27-Hydroxycholesterol Increase S100A8 and RAGE Expression in the Brain: a Link Between Cholesterol, Alarmins, and Neurodegeneration

MOLECULAR NEUROBIOLOGY (2021)

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Journal

MOLECULAR NEUROBIOLOGY
Volume 58, Issue 12, Pages 6063-6076

Publisher

SPRINGER
DOI: 10.1007/s12035-021-02521-8

Keywords

Alarmins; Astrocytes; Retinoid receptors; Oxysterols; Alzheimer's disease; Sterile inflammation

Categories

Neurosciences

Funding

  1. Swedish Brain Power
  2. Stockholm County Council
  3. Karolinska Institutet
  4. Margaretha af Ugglas Foundation
  5. Gun och Bertil Stohnes Stiftelse
  6. Karolinska Institutet fund for geriatric research
  7. Stiftelsen Gamla Tjanarinnor
  8. Demensfonden
  9. Hjarnfonden
  10. Alzheimerfonden
  11. Mexico's National Council for Science and Technology (CONACYT) CVU [209252]
  12. Olle Enqvist Foundation [2014/778]
  13. Ramon Areces Foundation, Spain
  14. EMBO Long-Term Fellowship [ALTF 696-2013]
  15. SSMF postdoctoral fellowship
  16. Juan de la Cierva-Incorporacion [IJCI-2016-27,658]
  17. Strategic Neuroscience Program
  18. Lindhes Advokatbyra

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This study demonstrates that hypercholesterolemia leads to S100A8 alarmin signaling in the brain through the cholesterol metabolite 27-OH, mediated by the nuclear receptor RXR gamma in both neurons and astrocytes. This suggests that 27-OH may play a detrimental role in the brain under conditions of high cholesterol levels.
Alterations in cholesterol metabolism in the brain have a major role in the physiology of Alzheimer's disease (AD). Oxysterols are cholesterol metabolites with multiple implications in memory functions and in neurodegeneration. Previous studies have shown detrimental effects of cholesterol metabolites in neurons, but its effect in glial cells is unknown. We used a high-fat/high-cholesterol diet in mice to study the effects of hypercholesterolemia over the alarmin S100A8 cascade in the hippocampus. Using CYP27Tg, a transgenic mouse model, we show that the hypercholesterolemia influence on the brain is mediated by the excess of 27-hydroxycholesterol (27-OH), a cholesterol metabolite. We also employed an acute model of 27-OH intraventricular injection in the brain to study RAGE and S100A8 response. We used primary cultures of neurons and astrocytes to study the effect of high levels of 27-OH over the S100A8 alarmin cascade. We report that a high-fat/high-cholesterol diet leads to an increase in S100A8 production in the brain. In CYP27Tg, we report an increase of S100A8 and its receptor RAGE in the hippocampus under elevated 27-OH in the brain. Using siRNA, we found that 27-OH upregulation of RAGE in astrocytes and neurons is mediated by the nuclear receptor RXR gamma. Silencing RXR gamma in neurons prevented 27-OH-mediated upregulation of RAGE. These results show that S100A8 alarmin and RAGE respond to high levels of 27-OH in the brain in both neurons and astrocytes through RXR gamma. Our study supports the notion that 27-OH mediates detrimental effects of hypercholesterolemia to the brain via alarmin signaling.

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