Versatile and simple approach to determine astrocyte territories in mouse neocortex and hippocampus

Antje Grosche; Jens Grosche; Mark Tackenberg; Dorit Scheller; Gwendolyn Gerstner; Annett Gumprecht; Thomas Pannicke; Petra G Hirrlinger; Ulrika Wilhelmsson; Kerstin Hüttmann; Wolfgang Härtig; Christian Steinhäuser; Milos Pekny; Andreas Reichenbach

doi:10.1371/journal.pone.0069143

Versatile and simple approach to determine astrocyte territories in mouse neocortex and hippocampus

PLoS One. 2013 Jul 23;8(7):e69143. doi: 10.1371/journal.pone.0069143. Print 2013.

Authors

Antje Grosche¹, Jens Grosche, Mark Tackenberg, Dorit Scheller, Gwendolyn Gerstner, Annett Gumprecht, Thomas Pannicke, Petra G Hirrlinger, Ulrika Wilhelmsson, Kerstin Hüttmann, Wolfgang Härtig, Christian Steinhäuser, Milos Pekny, Andreas Reichenbach

Affiliation

¹ Paul Flechsig Institute of Brain Research, Faculty of Medicine, University of Leipzig, Leipzig, Germany. antje.grosche@klinik.uni-regensburg.de

Abstract

Background: Besides their neuronal support functions, astrocytes are active partners in neuronal information processing. The typical territorial structure of astrocytes (the volume of neuropil occupied by a single astrocyte) is pivotal for many aspects of glia-neuron interactions.

Methods: Individual astrocyte territorial volumes are measured by Golgi impregnation, and astrocyte densities are determined by S100β immunolabeling. These data are compared with results from conventionally applied methods such as dye filling and determination of the density of astrocyte networks by biocytin loading. Finally, we implemented our new approach to investigate age-related changes in astrocyte territories in the cortex and hippocampus of 5- and 21-month-old mice.

Results: The data obtained by our simplified approach based on Golgi impregnation were compared to previously published dye filling experiments, and yielded remarkably comparable results regarding astrocyte territorial volumes. Moreover, we found that almost all coupled astrocytes (as indicated by biocytin loading) were immunopositive for S100β. A first application of this new experimental approach gives insight in age-dependent changes in astrocyte territorial volumes. They increased with age, while cell densities remained stable. In 5-month-old mice, the overlap factor was close to 1, revealing little or no interdigitation of astrocyte territories. However, in 21-month-old mice, the overlap factor was more than 2, suggesting that processes of adjacent astrocytes interdigitate.

Conclusion: Here we verified the usability of a simple, versatile method for assessing astrocyte territories and the overlap factor between adjacent territories. Second, we found that there is an age-related increase in territorial volumes of astrocytes that leads to loss of the strict organization in non-overlapping territories. Future studies should elucidate the physiological relevance of this adaptive reaction of astrocytes in the aging brain and the methods presented in this study might be a powerful tool to do so.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Aging / metabolism
Animals
Astrocytes / cytology*
Astrocytes / metabolism
Cell Count
Cell Size*
Cytological Techniques / methods*
Female
Golgi Apparatus / metabolism
Hippocampus / cytology*
Male
Mice
Neocortex / cytology*
Reproducibility of Results
S100 Proteins / metabolism
Staining and Labeling

Substances

S100 Proteins

Grants and funding

The work was supported by Deutsche Forschungsgemeinschaft (FOR 748 to AG and AR, GRK 1097 and RE 849/16-1 to AR, SPP 1172 to AR and CS, PA 615/2-1 to TP. SFB/TR3 to CS), the European Community (FP7-202167 NeuroGlia to CS), the Swedish Medical Research Council (project 11548), AFA Research Foundation, ALF Göteborg (project 11392), Sten A. Olsson Foundation for Research and Culture, Söderberg Foundations, Hjärnfonden, Hagströmer's Foundation Millenium, the Free Mason Foundation, Amlöv's Foundation, NanoNet COST Action (BM1002), the EU FP 7 Program EduGlia (237956 to A.R. and M.P.) and the EU FP 7 Program TargetBraIn (279017 to M.P.). The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.