| Literature DB >> 30166321 |
Grazyna Kwapiszewska1,2,3, Anna Gungl2, Jochen Wilhelm4,5, Leigh M Marsh1, Helene Thekkekara Puthenparampil1, Katharina Sinn6, Miroslava Didiasova7, Walter Klepetko6, Djuro Kosanovic4, Ralph T Schermuly4,5, Lukasz Wujak7, Benjamin Weiss8, Liliana Schaefer9, Marc Schneider10,5, Michael Kreuter11,5, Andrea Olschewski1, Werner Seeger4,5, Horst Olschewski1,12, Malgorzata Wygrecka7,5,3.
Abstract
Despite the beneficial effects of pirfenidone in treating idiopathic pulmonary fibrosis (IPF), it remains unclear if lung fibroblasts (FB) are the main therapeutic target.To resolve this question, we employed a comparative transcriptomic approach and analysed lung homogenates (LH) and FB derived from IPF patients treated with or without pirfenidone.In FB, pirfenidone therapy predominantly affected growth and cell division pathways, indicating a major cellular metabolic shift. In LH samples, pirfenidone treatment was mostly associated with inflammation-related processes. In FB and LH, regulated genes were over-represented in the Gene Ontology node "extracellular matrix". We identified lower expression of cell migration-inducing and hyaluronan-binding protein (CEMIP) in both LH and FB from pirfenidone-treated IPF patients. Plasma levels of CEMIP were elevated in IPF patients compared to healthy controls and decreased after 7 months of pirfenidone treatment. CEMIP expression in FB was downregulated in a glioma-associated oncogene homologue-dependent manner and CEMIP silencing in IPF FB reduced collagen production and attenuated cell proliferation and migration.Cumulatively, our approach indicates that pirfenidone exerts beneficial effects via its action on multiple pathways in both FB and other pulmonary cells, through its ability to control extracellular matrix architecture and inflammatory reactions.Entities:
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Year: 2018 PMID: 30166321 DOI: 10.1183/13993003.00564-2018
Source DB: PubMed Journal: Eur Respir J ISSN: 0903-1936 Impact factor: 16.671