Zhang, YunYunZhangZhu, HonglinHonglinZhuLayritz, FlorianFlorianLayritzLuo, HuiHuiLuoWohlfahrt, ThomasThomasWohlfahrtChen, Chih-WeiChih-WeiChenSoare, AlinaAlinaSoareBergmann, ChristinaChristinaBergmannRamming, AndreasAndreasRammingGroeber-Becker, FlorianFlorianGroeber-BeckerReuter, ChristianChristianReuterFornasini, GianFrancoGianFrancoFornasiniSoukhareva, NadejdaNadejdaSoukharevaSchreiber, BrianBrianSchreiberRamamurthy, SantoshSantoshRamamurthyAmann, KerstinKerstinAmannSchett, GeorgGeorgSchettDistler, Jörg H.WJörg H.WDistler2022-03-062022-03-062020https://publica.fraunhofer.de/handle/publica/26467510.1002/art.41259Objective Systemic sclerosis (SSc) is characterized by fibrosis, vascular disease, and inflammation. Adenosine signaling plays a central role in fibroblast activation. We undertook this study to evaluate the therapeutic effects of adenosine depletion with PEGylated adenosine deaminase (PEG&#8208;ADA) in preclinical models of SSc. Methods The effects of PEG&#8208;ADA on inflammation, vascular remodeling, and tissue fibrosis were analyzed in Fra&#8208;2 mice and in a B10.D2RTBALB/c (H&#8208;2d) model of sclerodermatous chronic graft&#8208;versus&#8208;host disease (GVHD). The effects of PEG&#8208;ADA were confirmed in vitro in a human full&#8208;thickness skin model. Results PEG&#8208;ADA effectively inhibited myofibroblast differentiation and reduced pulmonary fibrosis by 34.3% (with decreased collagen expression) (P = 0.0079; n = 6), dermal fibrosis by 51.8% (P = 0.0006; n = 6), and intestinal fibrosis by 17.7% (P = 0.0228; n = 6) in Fra&#8208;2 mice. Antifibrotic effects of PEG&#8208;ADA were also demonstrated in sclerodermatous chronic GVHD (reduced by 38.4%) (P = 0.0063; n = 8), and in a human full&#8208;thickness skin model. PEG&#8208;ADA treatment decreased inflammation and corrected the M2/Th2/group 2 innate lymphoid cell 2 bias. Moreover, PEG&#8208;ADA inhibited proliferation of pulmonary vascular smooth muscle cells (reduced by 40.5%) (P < 0.0001; n = 6), and prevented thickening of the vessel walls (reduced by 39.6%) (P = 0.0028; n = 6) and occlusions of pulmonary arteries (reduced by 63.9%) (P = 0.0147; n = 6). Treatment with PEG&#8208;ADA inhibited apoptosis of microvascular endothelial cells (reduced by 65.4%) (P = 0.0001; n = 6) and blunted the capillary rarefication (reduced by 32.5%) (P = 0.0199; n = 6). RNA sequencing demonstrated that treatment with PEG&#8208;ADA normalized multiple pathways related to fibrosis, vasculopathy, and inflammation in Fra&#8208;2 mice. Conclusion Treatment with PEG&#8208;ADA ameliorates the 3 cardinal features of SSc in pharmacologically relevant and well&#8208;tolerated doses. These findings may have direct translational implications, as PEG&#8208;ADA has already been approved by the Food and Drug Administration for the treatment of patients with ADA&#8208;deficient severe combined immunodeficiency disease.enadenosine deaminasecollagentranscription factor Fra 2systemic sclerosisskin fibrosis666660616610620journal article