Diverse Requirements for Microglial Survival, Specification, and Function Revealed by Defined-Medium Cultures

Overview

Journal Neuron

Publisher Cell Press

Specialty Neurology

Date 2017 May 19

PMID 28521131

Citations 292

Authors

Christopher J Bohlen

F Chris Bennett

Andrew F Tucker

Hannah Y Collins

Sara B Mulinyawe

Ben A Barres

Affiliations

Soon will be listed here.

Abstract

Microglia, the resident macrophages of the CNS, engage in various CNS-specific functions that are critical for development and health. To better study microglia and the properties that distinguish them from other tissue macrophage populations, we have optimized serum-free culture conditions to permit robust survival of highly ramified adult microglia under defined-medium conditions. We find that astrocyte-derived factors prevent microglial death ex vivo and that this activity results from three primary components, CSF-1/IL-34, TGF-β2, and cholesterol. Using microglial cultures that have never been exposed to serum, we demonstrate a dramatic and lasting change in phagocytic capacity after serum exposure. Finally, we find that mature microglia rapidly lose signature gene expression after isolation, and that this loss can be reversed by engrafting cells back into an intact CNS environment. These data indicate that the specialized gene expression profile of mature microglia requires continuous instructive signaling from the intact CNS.

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