International Journal of Molecular Sciences (May 2023)

TREM2 Expression and Amyloid-Beta Phagocytosis in Alzheimer’s Disease

  • Francesca La Rosa,
  • Simone Agostini,
  • Federica Piancone,
  • Ivana Marventano,
  • Ambra Hernis,
  • Chiara Fenoglio,
  • Daniela Galimberti,
  • Elio Scarpini,
  • Marina Saresella,
  • Mario Clerici

DOI
https://doi.org/10.3390/ijms24108626
Journal volume & issue
Vol. 24, no. 10
p. 8626

Abstract

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Alzheimer’s Disease is the most common form of dementia; its key pathological findings include the deposition of extracellular-neurotoxic-plaques composed of amyloid-beta (Ab). AD-pathogenesis involves mechanisms that operate outside the brain, and new researches indicate that peripheral inflammation is an early event in the disease. Herein, we focus on a receptor known as triggering-receptor-expressed-on-myeloid-cells2 (TREM2), which promotes the optimal immune cells function required to attenuate AD-progression and is, therefore, a potential target as peripheral diagnostic and prognostic-biomarker for Alzheimer’s Disease. The objective of this exploratory study was to analyze: (1) soluble-TREM2 (sTREM2) plasma and cerebrospinal fluid concentration, (2) TREM2-mRNA, (3) the percentage of TREM2-expressing monocytes, and (4) the concentration of miR-146a-5p and miR-34a-5p suspected to influence TREM2 transcription. Experiments were performed on PBMC collected by 15AD patients and 12age-matched healthy controls that were unstimulated or treated in inflammatory (LPS) conditions and Ab42 for 24 h; Aβ42-phagocytosis was also analyzed by AMNIS FlowSight. Results although preliminary, due to limitations by the small sample-size, showed that in AD compared to HC: TREM2 expressing monocytes were reduced, plasma sTREM2 concentration and TREM2-mRNA were significantly upregulated and Ab42-phagocytosis was diminished (for all p p = 0.02) as well in PBMC of AD, and miR-146 was only observed in AD cells (p = 0.0001).

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