Systems-based identification of the Hippo pathway for promoting fibrotic mesenchymal differentiation in systemic sclerosis

Author:

Ma FeiyangORCID,Tsou Pei-Suen,Gharaee-Kermani Mehrnaz,Plazyo Olesya,Xing Xianying,Kirma Joseph,Wasikowski RachaelORCID,Hile Grace A.,Harms Paul W.ORCID,Jiang Yanyun,Xing EnzeORCID,Nakamura Mio,Ochocki Danielle,Brodie William D.,Pillai ShivORCID,Maverakis Emanual,Pellegrini MatteoORCID,Modlin Robert L.ORCID,Varga John,Tsoi Lam C.,Lafyatis RobertORCID,Kahlenberg J. MichelleORCID,Billi Allison C.ORCID,Khanna DineshORCID,Gudjonsson Johann E.ORCID

Abstract

AbstractSystemic sclerosis (SSc) is a devastating autoimmune disease characterized by excessive production and accumulation of extracellular matrix, leading to fibrosis of skin and other internal organs. However, the main cellular participants in SSc skin fibrosis remain incompletely understood. Here using differentiation trajectories at a single cell level, we demonstrate a dual source of extracellular matrix deposition in SSc skin from both myofibroblasts and endothelial-to-mesenchymal-transitioning cells (EndoMT). We further define a central role of Hippo pathway effectors in differentiation and homeostasis of myofibroblast and EndoMT, respectively, and show that myofibroblasts and EndoMTs function as central communication hubs that drive key pro-fibrotic signaling pathways in SSc. Together, our data help characterize myofibroblast differentiation and EndoMT phenotypes in SSc skin, and hint that modulation of the Hippo pathway may contribute in reversing the pro-fibrotic phenotypes in myofibroblasts and EndoMTs.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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