Stem Cell Reports (Dec 2017)

Coupling between Myogenesis and Angiogenesis during Skeletal Muscle Regeneration Is Stimulated by Restorative Macrophages

  • Claire Latroche,
  • Michèle Weiss-Gayet,
  • Laurent Muller,
  • Cyril Gitiaux,
  • Pascal Leblanc,
  • Sophie Liot,
  • Sabrina Ben-Larbi,
  • Rana Abou-Khalil,
  • Nicolas Verger,
  • Paul Bardot,
  • Mélanie Magnan,
  • Fabrice Chrétien,
  • Rémi Mounier,
  • Stéphane Germain,
  • Bénédicte Chazaud

Journal volume & issue
Vol. 9, no. 6
pp. 2018 – 2033

Abstract

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Summary: In skeletal muscle, new functions for vessels have recently emerged beyond oxygen and nutrient supply, through the interactions that vascular cells establish with muscle stem cells. Here, we demonstrate in human and mouse that endothelial cells (ECs) and myogenic progenitor cells (MPCs) interacted together to couple myogenesis and angiogenesis in vitro and in vivo during skeletal muscle regeneration. Kinetics of gene expression of ECs and MPCs sorted at different time points of regeneration identified three effectors secreted by both ECs and MPCs. Apelin, Oncostatin M, and Periostin were shown to control myogenesis/angiogenesis coupling in vitro and to be required for myogenesis and vessel formation during muscle regeneration in vivo. Furthermore, restorative macrophages, which have been previously shown to support myogenesis in vivo, were shown in a 3D triculture model to stimulate myogenesis/angiogenesis coupling, notably through Oncostatin M production. Our data demonstrate that restorative macrophages orchestrate muscle regeneration by controlling myogenesis/angiogenesis coupling. : In this study, Chazaud et al. demonstrate that endothelial cells (ECs) and myogenic progenitor cells (MPCs) interacted to couple myogenesis and angiogenesis during skeletal muscle regeneration. EC- and MPC-derived Apelin, Oncostatin M, and Periostin controlled myogenesis/angiogenesis coupling and were required for myogenesis and vessel formation. They show that, via the production of Oncostatin M, restorative macrophages promoted myogenesis/angiogenesis coupling. Keywords: muscle stem cells, myogenesis, angiogenesis, skeletal muscle regeneration, macrophages