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Transient microglial absence assists postmigratory cortical neurons in proper differentiation.


ABSTRACT: In the developing cortex, postmigratory neurons accumulate in the cortical plate (CP) to properly differentiate consolidating subtype identities. Microglia, despite their extensive surveying activity, temporarily disappear from the midembryonic CP. However, the mechanism and significance of this absence are unknown. Here, we show that microglia bidirectionally migrate via attraction by CXCL12 released from the meninges and subventricular zone and thereby exit the midembryonic CP. Upon nonphysiological excessive exposure to microglia in vivo or in vitro, young postmigratory and in vitro-grown CP neurons showed abnormal differentiation with disturbed expression of the subtype-associated transcription factors and genes implicated in functional neuronal maturation. Notably, this effect is primarily attributed to interleukin 6 and type I interferon secreted by microglia. These results suggest that "sanctuarization" from microglia in the midembryonic CP is required for neurons to appropriately fine-tune the expression of molecules needed for proper differentiation, thus securing the establishment of functional cortical circuit.

SUBMITTER: Hattori Y 

PROVIDER: S-EPMC7118101 | biostudies-literature | 2020 Apr

REPOSITORIES: biostudies-literature

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Transient microglial absence assists postmigratory cortical neurons in proper differentiation.

Hattori Yuki Y   Naito Yu Y   Tsugawa Yoji Y   Nonaka Shigenori S   Wake Hiroaki H   Nagasawa Takashi T   Kawaguchi Ayano A   Miyata Takaki T  

Nature communications 20200402 1


In the developing cortex, postmigratory neurons accumulate in the cortical plate (CP) to properly differentiate consolidating subtype identities. Microglia, despite their extensive surveying activity, temporarily disappear from the midembryonic CP. However, the mechanism and significance of this absence are unknown. Here, we show that microglia bidirectionally migrate via attraction by CXCL12 released from the meninges and subventricular zone and thereby exit the midembryonic CP. Upon nonphysiol  ...[more]

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