Literature DB >> 26260923

Validation of Flow Cytometry and Magnetic Bead-Based Methods to Enrich CNS Single Cell Suspensions for Quiescent Microglia.

T A Volden1, C D Reyelts1, T A Hoke1, J Arikkath2, S J Bonasera3,4.   

Abstract

Microglia are resident mononuclear phagocytes within the CNS parenchyma that intimately interact with neurons and astrocytes to remodel synapses and extracellular matrix. We briefly review studies elucidating the molecular pathways that underlie microglial surveillance, activation, chemotaxis, and phagocytosis; we additionally place these studies in a clinical context. We describe and validate an inexpensive and simple approach to obtain enriched single cell suspensions of quiescent parenchymal and perivascular microglia from the mouse cerebellum and hypothalamus. Following preparation of regional CNS single cell suspensions, we remove myelin debris, and then perform two serial enrichment steps for cells expressing surface CD11b. Myelin depletion and CD11b enrichment are both accomplished using antigen-specific magnetic beads in an automated cell separation system. Flow cytometry of the resultant suspensions shows a significant enrichment for CD11b(+)/CD45(+) cells (perivascular microglia) and CD11b(+)/CD45(-) cells (parenchymal microglia) compared to starting suspensions. Of note, cells from these enriched suspensions minimally express Aif1 (aka Iba1), suggesting that the enrichment process does not evoke significant microglial activation. However, these cells readily respond to a functional challenge (LPS) with significant changes in the expression of molecules specifically associated with microglia. We conclude that methods employing a combination of magnetic-bead based sorting and flow cytometry produce suspensions highly enriched for microglia that are appropriate for a variety of molecular and cellular assays.

Entities:  

Keywords:  Magnetic bead-based cell separation; Microglia, flow cytometry; Microglia, purification; RT-qPCR

Mesh:

Substances:

Year:  2015        PMID: 26260923      PMCID: PMC4662612          DOI: 10.1007/s11481-015-9628-7

Source DB:  PubMed          Journal:  J Neuroimmune Pharmacol        ISSN: 1557-1890            Impact factor:   4.147


  87 in total

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8.  Normal adult ramified microglia separated from other central nervous system macrophages by flow cytometric sorting. Phenotypic differences defined and direct ex vivo antigen presentation to myelin basic protein-reactive CD4+ T cells compared.

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9.  Fcgamma receptors contribute to pyramidal cell death in the mouse hippocampus following local kainic acid injection.

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  1 in total

1.  Age-related changes in cerebellar and hypothalamic function accompany non-microglial immune gene expression, altered synapse organization, and excitatory amino acid neurotransmission deficits.

Authors:  Stephen J Bonasera; Jyothi Arikkath; Michael D Boska; Tammy R Chaudoin; Nicholas W DeKorver; Evan H Goulding; Traci A Hoke; Vahid Mojtahedzedah; Crystal D Reyelts; Balasrinivasa Sajja; A Katrin Schenk; Laurence H Tecott; Tiffany A Volden
Journal:  Aging (Albany NY)       Date:  2016-09-20       Impact factor: 5.682

  1 in total

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