Flow cytometric characterization of brain dendritic cell subsets after murine stroke

Flow cytometric characterization of brain dendritic cell subsets after murine stroke

Sterile inflammation is a substantial element of post-stroke pathophysiology with the determination of autoimmunity versus tolerance being one of its most important aspects. It is believed that this determination is initiated relatively early after stroke onset by clearing macrophages and migratory...

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Bibliographic Details
Published in:Experimental & translational stroke medicine Vol. 6; no. 1; p. 11
Main Authors: Pösel, Claudia, Uri, Anna, Schulz, Isabell, Boltze, Johannes, Weise, Gesa, Wagner, Daniel-Christoph
Format: Journal Article
Language:English
Published: England BioMed Central Ltd 04-11-2014
BioMed Central
Subjects:
Antigen presenting cells
Development and progression
Physiological aspects
Short Report
Stroke (Disease)
Germany
Brain ischemia
Flow cytometry
Dendritic cells
Macrophages
Cerebral stroke
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Summary:Sterile inflammation is a substantial element of post-stroke pathophysiology with the determination of autoimmunity versus tolerance being one of its most important aspects. It is believed that this determination is initiated relatively early after stroke onset by clearing macrophages and migratory dendritic cells (DC). However, the phenotypic differentiation of macrophages and DC is intricate particularly in the disease context. Here, we utilized a set of surface markers used in mucosal immunity research to investigate the involvement of macrophages and DC subpopulations in post-stroke inflammation in mice. Photothrombotic stroke induced a significant increase of lineage (CD3, B220, Ly6G and CD49b) negative CD11b+ cells in the brain primarily consisting of F4/80+ macrophages and, to a lesser extent, F4/80-/CD11c-/CD11b+ monocytes and F4/80-/CD11c+ DC. The latter could be differentiated into the classical migratory DC subpopulations (CD11b+ and CD103+), but no CD4 or CD8+ DC were found. Finally, stroke caused a significant increase of CD11b/CD103 double-positive DC in the affected brain hemisphere. The surface marker combination used in this study allowed a phenotypic differentiation of macrophages and DC subpopulations after stroke, thus providing an important prerequisite to study post-stroke immunity and tolerance.
ISSN:2040-7378
2040-7378
1939-067X
DOI:10.1186/2040-7378-6-11