A potent inhibitor of PAI-1, MDI-2517, mitigates disease severity in a preclinical systemic sclerosis model
Enming J. Su, Pei-Suen Tsou, Mark Warnock, Natalya Subbotina, Kris Mann, Sirapa Vichaikul, Alyssa Rosek, Lisa Leung, Xianying Xing, Enze Xing, Olesya Plazyo, Rachael Bogle, Lam C. Tsoi, Cory D. Emal, Dinesh Khanna, John Varga, Thomas H. Sisson, Johann E. Gudjonsson, Daniel A. Lawrence
Enming J. Su, Pei-Suen Tsou, Mark Warnock, Natalya Subbotina, Kris Mann, Sirapa Vichaikul, Alyssa Rosek, Lisa Leung, Xianying Xing, Enze Xing, Olesya Plazyo, Rachael Bogle, Lam C. Tsoi, Cory D. Emal, Dinesh Khanna, John Varga, Thomas H. Sisson, Johann E. Gudjonsson, Daniel A. Lawrence
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Research Article Pulmonology

A potent inhibitor of PAI-1, MDI-2517, mitigates disease severity in a preclinical systemic sclerosis model

Abstract

Systemic sclerosis (SSc) is a complex and heterogeneous condition characterized by progressive fibrosis in multiple organs. Recent studies implicate plasminogen activator inhibitor-1 (PAI-1) in the pathogenesis of SSc, and PAI-1 is considered as a potential target for therapy. Here, using single-cell and spatial RNA-seq analysis of skin biopsies from 18 healthy individuals and 22 SSc patients, we found elevated PAI-1 colocalizing to myofibroblasts with enriched extracellular matrix–associated biological processes. Treatment of SSc dermal fibroblasts with the small-molecule PAI-1 inhibitor MDI-2517 reduced the expression of the profibrotic markers COL1A1 and ACTA2. To investigate the therapeutic potential of MDI-2517, we evaluated its efficacy in reducing fibrosis in a preclinical model of SSc. Treatment of mice with MDI-2517 significantly reduced both skin and lung fibrosis and was superior to treatment with either pirfenidone or mycophenolate mofetil. Additionally, MDI-2517 attenuated weight loss and significantly reduced the expression of key profibrotic markers. Compared with tiplaxtinin, another PAI-1 inhibitor previously shown to be effective in a model of SSc, MDI-2517 was found to have superior efficacy at a 10-fold lower dose. These findings highlight the role of PAI-1 in the pathogenesis of SSc, and the potential of MDI-2517 for the treatment of SSc.

Authors

Enming J. Su, Pei-Suen Tsou, Mark Warnock, Natalya Subbotina, Kris Mann, Sirapa Vichaikul, Alyssa Rosek, Lisa Leung, Xianying Xing, Enze Xing, Olesya Plazyo, Rachael Bogle, Lam C. Tsoi, Cory D. Emal, Dinesh Khanna, John Varga, Thomas H. Sisson, Johann E. Gudjonsson, Daniel A. Lawrence

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Figure 6

Skin trichrome staining from the comparator study of MDI-2517, MMF, and combined MMF plus MDI-2517.

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Skin trichrome staining from the comparator study of MDI-2517, MMF, and ...
Twelve-week-old male C57BL/6J mice were subcutaneously implanted with osmotic pumps that delivered 100 U/kg (total) of bleomycin or saline over 7 days. The pumps were then removed, and at that time the mice were placed on treatment chows (drug concentration in chow: vehicle, 0 mg/kg; MDI-2517 at 500 mg/kg; MMF at 1,000 mg/kg; or combined MDI-2517 at 500 mg/kg and MMF at 1,000 mg/kg). On day 28, skin tissues were prepared for histological analysis by Masson’s trichrome stain. (A) Saline pump control chow. (B) Saline pump MDI-2517 chow. (C) Bleomycin control chow (no treatment). (D) Bleomycin MDI-2517 chow. (E) Bleomycin MMF chow. (F) Bleomycin combined MMF and MDI-2517 chow. (G) Quantification of skin thickness from Masson’s trichrome–stained slides. Scale bars: 100 μm. Data are shown as mean ± SD; n is indicated in each figure by the individual data points (5 to 8); **P < 0.01, ***P < 0.001, ****P < 0.0001 by 1-way ANOVA.