Saracatinib, a Selective Src Kinase Inhibitor, Blocks Fibrotic Responses in Preclinical Models of Pulmonary Fibrosis

Farida Ahangari; Christine Becker; Daniel G Foster; Maurizio Chioccioli; Meghan Nelson; Keriann Beke; Xing Wang; Aurelien Justet; Taylor Adams; Benjamin Readhead; Carly Meador; Kelly Correll; Loukia N Lili; Helen M Roybal; Kadi-Ann Rose; Shuizi Ding; Thomas Barnthaler; Natalie Briones; Giuseppe DeIuliis; Jonas C Schupp; Qin Li; Norihito Omote; Yael Aschner; Lokesh Sharma; Katrina W Kopf; Björn Magnusson; Ryan Hicks; Anna Backmark; Charles S Dela Cruz; Ivan Rosas; Leslie P Cousens; Joel T Dudley; Naftali Kaminski; Gregory P Downey

doi:10.1164/rccm.202010-3832OC

Saracatinib, a Selective Src Kinase Inhibitor, Blocks Fibrotic Responses in Preclinical Models of Pulmonary Fibrosis

Am J Respir Crit Care Med. 2022 Dec 15;206(12):1463-1479. doi: 10.1164/rccm.202010-3832OC.

Authors

Farida Ahangari¹, Christine Becker^{2

3}, Daniel G Foster⁴, Maurizio Chioccioli¹, Meghan Nelson⁴, Keriann Beke⁴, Xing Wang^{2

3}, Aurelien Justet^{1

5}, Taylor Adams¹, Benjamin Readhead^{2

6}, Carly Meador⁴, Kelly Correll⁴, Loukia N Lili², Helen M Roybal⁴, Kadi-Ann Rose¹, Shuizi Ding¹, Thomas Barnthaler^{1

7}, Natalie Briones⁴, Giuseppe DeIuliis¹, Jonas C Schupp¹, Qin Li¹, Norihito Omote¹, Yael Aschner⁴, Lokesh Sharma¹, Katrina W Kopf⁴, Björn Magnusson⁸, Ryan Hicks⁹, Anna Backmark⁸, Charles S Dela Cruz¹, Ivan Rosas¹⁰, Leslie P Cousens¹¹, Joel T Dudley², Naftali Kaminski¹, Gregory P Downey⁴

Affiliations

¹ Section of Pulmonary, Critical Care, and Sleep Medicine, Department of Medicine, Yale University School of Medicine, New Haven, Connecticut.
² Institute for Next Generation Healthcare, Department of Genetics and Genomic Sciences, and.
³ Division of Clinical Immunology, Department of Medicine, Icahn School of Medicine at Mount Sinai, New York, New York.
⁴ Division of Pulmonary, Critical Care, and Sleep Medicine, Department of Medicine, Department of Pediatrics, and Department of Immunology and Genomic Medicine, National Jewish Health, Denver, Colorado.
⁵ Service de Pneumologie, UNICAEN, Normandie University, Caen, France.
⁶ ASU-Banner Neurodegenerative Disease Research Center, Arizona State University, Tempe, Arizona.
⁷ Section of Pharmacology, Otto Loewi Research Center, Medical University of Graz, Graz, Austria.
⁸ Discovery Biology, Discovery Sciences, Research & Development, AstraZeneca, Gothenburg, Sweden.
⁹ BioPharmaceuticals Research & Development Cell Therapy, Research, and Early Development, Cardiovascular, Renal, and Metabolism (CVRM), AstraZeneca, Gothenburg, Sweden.
¹⁰ Department of Medicine, Baylor College of Medicine, Houston, Texas; and.
¹¹ Emerging Innovations, Discovery Sciences, Research & Development, AstraZeneca, Boston, Massachusetts.

Abstract

Rationale: Idiopathic pulmonary fibrosis (IPF) is a chronic, progressive, and often fatal disorder. Two U.S. Food and Drug Administration-approved antifibrotic drugs, nintedanib and pirfenidone, slow the rate of decline in lung function, but responses are variable and side effects are common. Objectives: Using an in silico data-driven approach, we identified a robust connection between the transcriptomic perturbations in IPF disease and those induced by saracatinib, a selective Src kinase inhibitor originally developed for oncological indications. Based on these observations, we hypothesized that saracatinib would be effective at attenuating pulmonary fibrosis. Methods: We investigated the antifibrotic efficacy of saracatinib relative to nintedanib and pirfenidone in three preclinical models: 1) in vitro in normal human lung fibroblasts; 2) in vivo in bleomycin and recombinant Ad-TGF-β (adenovirus transforming growth factor-β) murine models of pulmonary fibrosis; and 3) ex vivo in mice and human precision-cut lung slices from these two murine models as well as patients with IPF and healthy donors. Measurements and Main Results: In each model, the effectiveness of saracatinib in blocking fibrogenic responses was equal or superior to nintedanib and pirfenidone. Transcriptomic analyses of TGF-β-stimulated normal human lung fibroblasts identified specific gene sets associated with fibrosis, including epithelial-mesenchymal transition, TGF-β, and WNT signaling that was uniquely altered by saracatinib. Transcriptomic analysis of whole-lung extracts from the two animal models of pulmonary fibrosis revealed that saracatinib reverted many fibrogenic pathways, including epithelial-mesenchymal transition, immune responses, and extracellular matrix organization. Amelioration of fibrosis and inflammatory cascades in human precision-cut lung slices confirmed the potential therapeutic efficacy of saracatinib in human lung fibrosis. Conclusions: These studies identify novel Src-dependent fibrogenic pathways and support the study of the therapeutic effectiveness of saracatinib in IPF treatment.

Keywords: Src family kinase; idiopathic pulmonary fibrosis; lung fibrosis; preclinical models; tyrosine kinase.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Animals
Bleomycin / adverse effects
Fibroblasts / metabolism
Fibrosis
Humans
Idiopathic Pulmonary Fibrosis* / drug therapy
Lung / pathology
Mice
Protein Kinase Inhibitors* / therapeutic use
Transforming Growth Factor beta / metabolism
src-Family Kinases / metabolism

Substances

Bleomycin
Protein Kinase Inhibitors
saracatinib
src-Family Kinases
Transforming Growth Factor beta

Abstract

Publication types

MeSH terms

Substances

Grants and funding