| Literature DB >> 34344890 |
Lise Rabiller1,2, Virginie Robert1, Adèle Arlat1,3, Elodie Labit1,4, Marielle Ousset1,3, Marie Salon5,3, Agnès Coste5,3, Léa Da Costa-Fernandes1,3, Paul Monsarrat1,3, Bruno Ségui6, Mireille André1,3, Christophe Guissard1,3, Marie-Laure Renoud1,3, Marine Silva7, Gilles Mithieux7, Isabelle Raymond-Letron1,3, Luc Pénicaud1, Anne Lorsignol1,3, Louis Casteilla1,3, Cécile Dromard Berthézène1,3, Béatrice Cousin8,9.
Abstract
Tissue repair after lesion usually leads to scar healing and thus loss of function in adult mammals. In contrast, other adult vertebrates such as amphibians have the ability to regenerate and restore tissue homeostasis after lesion. Understanding the control of the repair outcome is thus a concerning challenge for regenerative medicine. We recently developed a model of induced tissue regeneration in adult mice allowing the comparison of the early steps of regenerative and scar healing processes. By using studies of gain and loss of function, specific cell depletion approaches, and hematopoietic chimeras we demonstrate here that tissue regeneration in adult mammals depends on an early and transient peak of granulocyte producing reactive oxygen species and an efficient efferocytosis specifically by tissue-resident macrophages. These findings highlight key and early cellular pathways able to drive tissue repair towards regeneration in adult mammals.Entities:
Year: 2021 PMID: 34344890 DOI: 10.1038/s41536-021-00151-1
Source DB: PubMed Journal: NPJ Regen Med ISSN: 2057-3995