Phagocytic Properties of Microglia in Vitro: Implications for a Role in Multiple Sclerosis and EAE

Overview

Journal Microsc Res Tech

Specialty Radiology

Date 2001 Jul 17

PMID 11455615

Citations 40

Authors

M E Smith

Affiliations

Soon will be listed here.

Abstract

The microglial cell, after many years of neglect, has become recognized as the sole representative cell of the immune system that resides in the normal central nervous system. While normally dormant, microglia can be activated by secretory substances or signals associated with disease or injury, and becomes a phagocytic cell, which also produces its own injurious molecules. In the activating process, its morphology is changed from a resting process-bearing cell, into a rounded amoebic form, and displays new or increased amounts of functional markers, such as receptors and Class I and Class II MHC molecules. Microglia prepared from newborn mice or rats for tissue culture are already activated, and can be used for studies of their phagocytic properties. Although they can phagocytize foreign substances, their uptake and metabolism of myelin are emphasized here, in keeping with their role in demyelinating diseases. A number of receptors have been implicated and appear to be important in the attachment to, and ingestion of, myelin particles in vitro, including the Fc, complement, macrophage scavenger, and the Galectin-3/MAC-2 receptors, although the alpha2-macroglobulin/low-density lipoprotein receptor and mannose receptors have also been suggested as participants in myelin phagocytosis. Certain cytokines and adhesion molecules also regulate the phagocytic activity of microglia. Comparative in vitro studies of phagocytosis by peritoneal macrophages and microglia have shown that the two kinds of cells respond differently to regulatory molecules, and it is concluded that they have different innate properties. The role of microglia in the demyelinative diseases experimental autoimmune encephalomyelitis and multiple sclerosis is emphasized here, and the possible means of intervention in the process leading to myelin destruction is discussed. Published 2001 Wiley-Liss, Inc.

Citing Articles

Myeloid antigen-presenting cells in neurodegenerative diseases: a focus on classical and non-classical MHC molecules.

Afify R, Lipsius K, Wyatt-Johnson S, Brutkiewicz R Front Neurosci. 2024; 18:1488382.

PMID: 39720231 PMC: 11667120. DOI: 10.3389/fnins.2024.1488382.

Transplanting Microglia for Treating CNS Injuries and Neurological Diseases and Disorders, and Prospects for Generating Exogenic Microglia.

Var S, Strell P, Johnson S, Roman A, Vasilakos Z, Low W Cell Transplant. 2023; 32:9636897231171001.

PMID: 37254858 PMC: 10236244. DOI: 10.1177/09636897231171001.

The roles of microglia and astrocytes in myelin phagocytosis in the central nervous system.

Xu T, Liu C, Deng S, Gan L, Zhang Z, Yang G J Cereb Blood Flow Metab. 2022; 43(3):325-340.

PMID: 36324281 PMC: 9941857. DOI: 10.1177/0271678X221137762.

Complement-Mediated Microglial Phagocytosis and Pathological Changes in the Development and Degeneration of the Visual System.

Borucki D, Toutonji A, Couch C, Mallah K, Rohrer B, Tomlinson S Front Immunol. 2020; 11:566892.

PMID: 33072106 PMC: 7541817. DOI: 10.3389/fimmu.2020.566892.

Microglial responses after phagocytosis: Escherichia coli bioparticles, but not cell debris or amyloid beta, induce matrix metalloproteinase-9 secretion in cultured rat primary microglial cells.

Hamanaka G, Kubo T, Ohtomo R, Takase H, Reyes-Bricio E, Oribe S Glia. 2020; 68(7):1435-1444.

PMID: 32057146 PMC: 7256913. DOI: 10.1002/glia.23791.