Scientific Reports (Jul 2024)

Tunneling nanotube-driven complete regeneration of murine fetal skin

  • Yukari Nakajima,
  • Shuichi Obata,
  • Kento Takaya,
  • Shigeki Sakai,
  • Yushi Suzuki,
  • Keisuke Okabe,
  • Noriko Aramaki-Hattori,
  • Ryoichi Mori,
  • Yuichi Kadoya,
  • Kazuo Kishi

DOI
https://doi.org/10.1038/s41598-024-68083-6
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 12

Abstract

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Abstract This study investigated the three-dimensional (3D) cellular interactions and tunneling nanotubes (TNTs) during fetal mouse skin regeneration on embryonic days 13 (E13) and 15 (E15). We aimed to understand spatial relationships among cell types involved in skin regeneration and assess the potential role of TNTs. Full-thickness skin incisions were performed in E13 and E15 embryos. Wound sites were collected, embedded in epoxy resin, processed for 3D reconstruction (1 μm thickness sections), and subjected to whole-mount immunostaining. We conducted in vitro co-culture experiments with fetal macrophages and fibroblasts to observe TNT formation. To assess the effect of TNTs on skin regeneration, an inhibiting agent (cytochalasin B) was administered to amniotic fluid. Results revealed that E13 epidermal keratinocytes interacted with dermal fibroblasts and macrophages, facilitating skin regrowth. TNT structures were observed at the E13-cell wound sites, among macrophages, and between macrophages and fibroblasts, confirmed through in vitro co-culture experiments. In vitro and utero cytochalasin B administration hindered those formation and inefficient skin texture regeneration at E13 wound sites. This emphasizes the necessity of 3D cellular interactions between epidermal and dermal cells during skin regeneration in mouse embryos at E13. The prevalence of TNT structures indicated their involvement in achieving complete skin texture restoration.