| Literature DB >> 27411339 |
Ben J Gu1, Xin Huang2, Amber Ou2, Alan Rembach2, Christopher Fowler2, Pavan K Avula2, Adam Horton2, James D Doecke3, Victor L Villemagne2,4, S Lance Macaulay5, Paul Maruff2,6, Erica L Fletcher7, Robyn Guymer8, James S Wiley2, Colin L Masters2.
Abstract
Sporadic Alzheimer's disease (AD) is characterised by the deposition and accumulation of specific protein aggregates. Failure of clearance could underlie this process, and recent genetic association studies point towards involvement of the phagocytosis and autophagy pathways. We developed a real-time tri-color flow cytometry method to quantitate the phagocytic function of human peripheral blood monocyte subsets including non-classic CD14(dim)CD16(+), intermediate CD14(+)CD16(+) and classic CD14(+)CD16(-) monocytes. Using this method, we have measured the phagocytic ability of fresh monocytes in a study of preclinical, prodromal and clinical AD, matched with cognitively normal healthy control subjects. Basal levels of phagocytosis in all three subsets of monocytes were similar between healthy controls and AD patients, while a significant increase of basal phagocytosis was found in subjects with high Aβ-amyloid burden as assessed by PET scans. Pre-treating cells with Copaxone (CPX, to stimulate phagocytosis) or ATP (an inhibitor of P2X7-mediated phagocytosis) showed a differential response depending on clinical or Aβ-burden status, indicating a relative functional deficit. Overall the results are consistent with a perturbation of basal and stimulated innate phagocytosis in sporadic AD.Entities:
Keywords: ATP; Alzheimer’s disease; Copaxone (glatiramer acetate); P2X7; Phagocytosis
Mesh:
Substances:
Year: 2016 PMID: 27411339 DOI: 10.1007/s00401-016-1596-3
Source DB: PubMed Journal: Acta Neuropathol ISSN: 0001-6322 Impact factor: 17.088