Helmholtz Gemeinschaft

Search
Browse
Statistics
Feeds

Barreloid borders and neuronal activity shape panglial gap junction-coupled networks in the mouse thalamus

Item Type:Article
Title:Barreloid borders and neuronal activity shape panglial gap junction-coupled networks in the mouse thalamus
Creators Name:Claus, L., Philippot, C., Griemsmann, S., Timmermann, A., Jabs, R., Henneberger, C., Kettenmann, H. and Steinhaeuser, C.
Abstract:The ventral posterior nucleus of the thalamus plays an important role in somatosensory information processing. It contains elongated cellular domains called barreloids, which are the structural basis for the somatotopic organization of vibrissae representation. So far, the organization of glial networks in these barreloid structures and its modulation by neuronal activity has not been studied. We have developed a method to visualize thalamic barreloid fields in acute slices. Combining electrophysiology, immunohistochemistry, and electroporation in transgenic mice with cell type-specific fluorescence labeling, we provide the first structure-function analyses of barreloidal glial gap junction networks. We observed coupled networks, which comprised both astrocytes and oligodendrocytes. The spread of tracers or a fluorescent glucose derivative through these networks was dependent on neuronal activity and limited by the barreloid borders, which were formed by uncoupled or weakly coupled oligodendrocytes. Neuronal somata were distributed homogeneously across barreloid fields with their processes running in parallel to the barreloid borders. Many astrocytes and oligodendrocytes were not part of the panglial networks. Thus, oligodendrocytes are the cellular elements limiting the communicating panglial network to a single barreloid, which might be important to ensure proper metabolic support to active neurons located within a particular vibrissae signaling pathway.
Keywords:Astrocyte, Barreloid, Gap Junction Coupling, Oligodendrocyte, Thalamus, Animals, Mice
Source:Cerebral Cortex
ISSN:1047-3211
Publisher:Oxford University Press
Volume:28
Number:1
Page Range:213-222
Date:1 January 2018
Official Publication:https://doi.org/10.1093/cercor/bhw368
PubMed:View item in PubMed

Repository Staff Only: item control page

Open Access
MDC Library