Between Fate Choice and Self-Renewal-Heterogeneity of Adult Neural Crest-Derived Stem Cells

Anna L Höving; Beatrice A Windmöller; Cornelius Knabbe; Barbara Kaltschmidt; Christian Kaltschmidt; Johannes F W Greiner

doi:10.3389/fcell.2021.662754

Between Fate Choice and Self-Renewal-Heterogeneity of Adult Neural Crest-Derived Stem Cells

Front Cell Dev Biol. 2021 Apr 8:9:662754. doi: 10.3389/fcell.2021.662754. eCollection 2021.

Authors

Anna L Höving^{1

2}, Beatrice A Windmöller^{1

3}, Cornelius Knabbe^{2

3}, Barbara Kaltschmidt^{1

3

4}, Christian Kaltschmidt^{1

3}, Johannes F W Greiner^{1

3}

Affiliations

¹ Department of Cell Biology, University of Bielefeld, Bielefeld, Germany.
² Institute for Laboratory- and Transfusion Medicine, Heart and Diabetes Centre North Rhine-Westphalia (NRW), Ruhr University Bochum, Bad Oeynhausen, Germany.
³ Forschungsverbund BioMedizin Bielefeld FBMB e.V., Bielefeld, Germany.
⁴ Molecular Neurobiology, University of Bielefeld, Bielefeld, Germany.

Abstract

Stem cells of the neural crest (NC) vitally participate to embryonic development, but also remain in distinct niches as quiescent neural crest-derived stem cell (NCSC) pools into adulthood. Although NCSC-populations share a high capacity for self-renewal and differentiation resulting in promising preclinical applications within the last two decades, inter- and intrapopulational differences exist in terms of their expression signatures and regenerative capability. Differentiation and self-renewal of stem cells in developmental and regenerative contexts are partially regulated by the niche or culture condition and further influenced by single cell decision processes, making cell-to-cell variation and heterogeneity critical for understanding adult stem cell populations. The present review summarizes current knowledge of the cellular heterogeneity within NCSC-populations located in distinct craniofacial and trunk niches including the nasal cavity, olfactory bulb, oral tissues or skin. We shed light on the impact of intrapopulational heterogeneity on fate specifications and plasticity of NCSCs in their niches in vivo as well as during in vitro culture. We further discuss underlying molecular regulators determining fate specifications of NCSCs, suggesting a regulatory network including NF-κB and NC-related transcription factors like SLUG and SOX9 accompanied by Wnt- and MAPK-signaling to orchestrate NCSC stemness and differentiation. In summary, adult NCSCs show a broad heterogeneity on the level of the donor and the donors' sex, the cell population and the single stem cell directly impacting their differentiation capability and fate choices in vivo and in vitro. The findings discussed here emphasize heterogeneity of NCSCs as a crucial parameter for understanding their role in tissue homeostasis and regeneration and for improving their applicability in regenerative medicine.

Keywords: adult stem cells; fate choice; heterogeneity; neural crest; neural crest-derived stem cells; single cell analysis.

Publication types

Review