PLoS ONE (Jan 2013)

Stathmin regulates keratinocyte proliferation and migration during cutaneous regeneration.

  • Sabrina Schmitt,
  • Kai Safferling,
  • Kathi Westphal,
  • Manuel Hrabowski,
  • Ute Müller,
  • Peter Angel,
  • Lars Wiechert,
  • Volker Ehemann,
  • Benedikt Müller,
  • Stefan Holland-Cunz,
  • Damian Stichel,
  • Nathalie Harder,
  • Karl Rohr,
  • Günter Germann,
  • Franziska Matthäus,
  • Peter Schirmacher,
  • Niels Grabe,
  • Kai Breuhahn

DOI
https://doi.org/10.1371/journal.pone.0075075
Journal volume & issue
Vol. 8, no. 9
p. e75075

Abstract

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Cutaneous regeneration utilizes paracrine feedback mechanisms to fine-tune the regulation of epidermal keratinocyte proliferation and migration. However, it is unknown how fibroblast-derived hepatocyte growth factor (HGF) affects these mutually exclusive processes in distinct cell populations. We here show that HGF stimulates the expression and phosphorylation of the microtubule-destabilizing factor stathmin in primary human keratinocytes. Quantitative single cell- and cell population-based analyses revealed that basal stathmin levels are important for the migratory ability of keratinocytes in vitro; however, its expression is moderately induced in the migration tongue of mouse skin or organotypic multi-layered keratinocyte 3D cultures after full-thickness wounding. In contrast, clearly elevated stathmin expression is detectable in hyperproliferative epidermal areas. In vitro, stathmin silencing significantly reduced keratinocyte proliferation. Automated quantitative and time-resolved analyses in organotypic cocultures demonstrated a high correlation between Stathmin/phospho-Stathmin and Ki67 positivity in epidermal regions with proliferative activity. Thus, activation of stathmin may stimulate keratinocyte proliferation, while basal stathmin levels are sufficient for keratinocyte migration during cutaneous regeneration.