| Literature DB >> 34012116 |
Guillaume Hoeffel1, Guilhaume Debroas2, Anais Roger2, Rafaelle Rossignol2, Jordi Gouilly2, Caroline Laprie2, Lionel Chasson2, Pierre-Vincent Barbon2, Anaïs Balsamo2, Ana Reynders3, Aziz Moqrich3, Sophie Ugolini4.
Abstract
Inflammation is a defence response to tissue damage that requires tight regulation in order to prevent impaired healing. Tissue-resident macrophages have a key role in tissue repair1, but the precise molecular mechanisms that regulate the balance between inflammatory and pro-repair macrophage responses during healing remain poorly understood. Here we demonstrate a major role for sensory neurons in promoting the tissue-repair function of macrophages. In a sunburn-like model of skin damage in mice, the conditional ablation of sensory neurons expressing the Gαi-interacting protein (GINIP) results in defective tissue regeneration and in dermal fibrosis. Elucidation of the underlying molecular mechanisms revealed a crucial role for the neuropeptide TAFA4, which is produced in the skin by C-low threshold mechanoreceptors-a subset of GINIP+ neurons. TAFA4 modulates the inflammatory profile of macrophages directly in vitro. In vivo studies in Tafa4-deficient mice revealed that TAFA4 promotes the production of IL-10 by dermal macrophages after UV-induced skin damage. This TAFA4-IL-10 axis also ensures the survival and maintenance of IL-10+TIM4+ dermal macrophages, reducing skin inflammation and promoting tissue regeneration. These results reveal a neuroimmune regulatory pathway driven by the neuropeptide TAFA4 that promotes the anti-inflammatory functions of macrophages and prevents fibrosis after tissue damage, and could lead to new therapeutic perspectives for inflammatory diseases.Entities:
Mesh:
Substances:
Year: 2021 PMID: 34012116 DOI: 10.1038/s41586-021-03563-7
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962