Continuous live imaging of adult neural stem cell division and lineage progression in vitro

Author:

Costa Marcos R.12,Ortega Felipe3,Brill Monika S.3,Beckervordersandforth Ruth4,Petrone Ciro4,Schroeder Timm4,Götz Magdalena345,Berninger Benedikt34

Affiliation:

1. Instituto do Cérebro, Universidade Federal do Rio Grande do Norte (UFRN), 59072-970 Natal, Brazil

2. Edmond and Lily Safra International Institute of Neuroscience of Natal (ELS-IINN), 59066-060 Natal, Brazil

3. Department of Physiological Genomics, Institute of Physiology, Ludwig-Maximilians University Munich, Schillerstrasse 46, D-80336 Munich, Germany

4. Institute for Stem Cell Research, National Research Center for Environment and Health, Ingolstädter Landstrasse 1, D-85764 Neuherberg, Germany

5. Munich Center for Integrated Protein Science CiPSM, Butenandtstraße 5-13, Munich 81377, Germany

Abstract

Little is known about the intrinsic specification of adult neural stem cells (NSCs) and to what extent they depend on their local niche. To observe adult NSC division and lineage progression independent of their niche, we isolated cells from the adult mouse subependymal zone (SEZ) and cultured them at low density without growth factors. We demonstrate here that SEZ cells in this culture system are primarily neurogenic and that adult NSCs progress through stereotypic lineage trees consisting of asymmetric stem cell divisions, symmetric transit-amplifying divisions and final symmetric neurogenic divisions. Stem cells, identified by their astro/radial glial identity and their slow-dividing nature, were observed to generate asymmetrically and fast-dividing cells that maintained an astro/radial glia identity. These, in turn, gave rise to symmetrically and fast-dividing cells that lost glial hallmarks, but had not yet acquired neuronal features. The number of amplifying divisions was limited to a maximum of five in this system. Moreover, we found that cell growth correlated with the number of subsequent divisions of SEZ cells, with slow-dividing astro/radial glia exhibiting the most substantial growth prior to division. The fact that in the absence both of exogenously supplied growth factors and of signals provided by the local niche neurogenic lineage progression takes place in such stereotypic fashion, suggests that lineage progression is, to a significant degree, cell intrinsic or pre-programmed at the beginning of the lineage.

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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