EMBO Molecular Medicine (Aug 2021)

Pro‐inflammatory immunity supports fibrosis advancement in epidermolysis bullosa: intervention with Ang‐(1‐7)

  • Rocco Bernasconi,
  • Kerstin Thriene,
  • Elena Romero‐Fernández,
  • Christine Gretzmeier,
  • Tobias Kühl,
  • Mareike Maler,
  • Pauline Nauroy,
  • Svenja Kleiser,
  • Anne‐Catherine Rühl‐Muth,
  • Michael Stumpe,
  • Dimitra Kiritsi,
  • Stefan F Martin,
  • Boris Hinz,
  • Leena Bruckner‐Tuderman,
  • Jörn Dengjel,
  • Alexander Nyström

DOI
https://doi.org/10.15252/emmm.202114392
Journal volume & issue
Vol. 13, no. 10
pp. 1 – 20

Abstract

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Abstract Recessive dystrophic epidermolysis bullosa (RDEB), a genetic skin blistering disease, is a paradigmatic condition of tissue fragility‐driven multi‐organ fibrosis. Here, longitudinal analyses of the tissue proteome through the course of naturally developing disease in RDEB mice revealed that increased pro‐inflammatory immunity associates with fibrosis evolution. Mechanistically, this fibrosis is a consequence of altered extracellular matrix organization rather than that of increased abundance of major structural proteins. In a humanized system of disease progression, we targeted inflammatory cell fibroblast communication with Ang‐(1‐7)—an anti‐inflammatory heptapeptide of the renin‐angiotensin system, which reduced the fibrosis‐evoking aptitude of RDEB cells. In vivo, systemic administration of Ang‐(1‐7) efficiently attenuated progression of multi‐organ fibrosis and increased survival of RDEB mice. Collectively, our study shows that selective down‐modulation of pro‐inflammatory immunity may mitigate injury‐induced fibrosis. Furthermore, together with published data, our data highlight molecular diversity among fibrotic conditions. Both findings have direct implications for the design of therapies addressing skin fragility and fibrosis.

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