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Tissue-resident macrophages can be generated de novo in adult human skin from resident progenitor cells during substance P-mediated neurogenic inflammation ex vivo

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Listed:
  • Jennifer Gherardini
  • Youhei Uchida
  • Jonathan A Hardman
  • Jérémy Chéret
  • Kimberly Mace
  • Marta Bertolini
  • Ralf Paus

Abstract

Besides monocyte (MO)-derived macrophages (MACs), self-renewing tissue-resident macrophages (trMACs) maintain the intracutaneous MAC pool in murine skin. Here, we have asked whether the same phenomenon occurs in human skin using organ-cultured, full-thickness skin detached from blood circulation and bone marrow. Skin stimulation ex vivo with the neuropeptide substance P (SP), mimicking neurogenic skin inflammation, significantly increased the number of CD68+MACs in the papillary dermis without altering intracutaneous MAC proliferation or apoptosis. Since intraluminal CD14+MOs were undetectable in the non-perfused dermal vasculature, new MACs must have differentiated from resident intracutaneous progenitor cells in human skin. Interestingly, CD68+MACs were often seen in direct cell-cell-contact with cells expressing both, the hematopoietic stem cell marker CD34 and SP receptor (neurokinin-1 receptor [NK1R]). These cell-cell contacts and CD34+cell proliferation were up-regulated in SP-treated skin samples. Collectively, our study provides the first evidence that resident MAC progenitors, from which mature MACs can rapidly differentiate within the tissue, do exist in normal adult human skin. That these NK1R+trMAC-progenitor cells quickly respond to a key stress-associated neuroinflammatory stimulus suggests that this may satisfy increased local MAC demand under conditions of wounding/stress.

Suggested Citation

  • Jennifer Gherardini & Youhei Uchida & Jonathan A Hardman & Jérémy Chéret & Kimberly Mace & Marta Bertolini & Ralf Paus, 2020. "Tissue-resident macrophages can be generated de novo in adult human skin from resident progenitor cells during substance P-mediated neurogenic inflammation ex vivo," PLOS ONE, Public Library of Science, vol. 15(1), pages 1-16, January.
  • Handle: RePEc:plo:pone00:0227817
    DOI: 10.1371/journal.pone.0227817
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    1. Calum C. Bain & Catherine A. Hawley & Hannah Garner & Charlotte L. Scott & Anika Schridde & Nicholas J. Steers & Matthias Mack & Anagha Joshi & Martin Guilliams & Allan Mc I. Mowat & Frederic Geissman, 2016. "Long-lived self-renewing bone marrow-derived macrophages displace embryo-derived cells to inhabit adult serous cavities," Nature Communications, Nature, vol. 7(1), pages 1-14, September.
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