Pirfenidone exacerbates Th2-driven vasculopathy in a mouse model of systemic sclerosis-associated interstitial lung disease

Anna Birnhuber; Katharina Jandl; Valentina Biasin; Elisabeth Fließer; Francesco Valzano; Leigh M. Marsh; Christina Krolczik; Andrea Olschewski; Jochen Wilhelm; Wolfgang Toller; Akos Heinemann; Horst Olschewski; Malgorzata Wygrecka; Grazyna Kwapiszewska

doi:10.1183/13993003.02347-2021

Pirfenidone exacerbates Th2-driven vasculopathy in a mouse model of systemic sclerosis-associated interstitial lung disease

Anna Birnhuber
, Katharina Jandl
, Valentina Biasin
, Elisabeth Fließer
, Francesco Valzano
, Leigh M. Marsh
, Christina Krolczik
, Andrea Olschewski
, Jochen Wilhelm
, Wolfgang Toller
, Akos Heinemann
, Horst Olschewski
, Malgorzata Wygrecka
, Grazyna Kwapiszewska^*

^*Corresponding author for this work

Research output: Journal article (peer-reviewed) › Journal article

21 Citations (Scopus)

Abstract

Background Systemic sclerosis (SSc) is an autoimmune disease characterised by severe vasculopathy and fibrosis of various organs including the lung. Targeted treatment options for SSc-associated interstitial lung disease (SSc-ILD) are scarce. We assessed the effects of pirfenidone in a mouse model of SSc-ILD. Methods Pulmonary function, inflammation and collagen deposition in response to pirfenidone were assessed in Fra-2-overexpressing transgenic (Fra-2 TG) and bleomycin-treated mice. In Fra-2 TG mice, lung transcriptome was analysed after pirfenidone treatment. In vitro, pirfenidone effects on human eosinophil and endothelial cell function were analysed using flow cytometry-based assays and electric cell-substrate impedance measurements, respectively. Results Pirfenidone treatment attenuated pulmonary remodelling in the bleomycin model, but aggravated pulmonary inflammation, fibrosis and vascular remodelling in Fra-2 TG mice. Pirfenidone increased interleukin (IL)-4 levels and eosinophil numbers in lung tissue of Fra-2 TG mice without directly affecting eosinophil activation and migration in vitro. A pronounced immune response with high levels of cytokines/ chemokines and disturbed endothelial integrity with low vascular endothelial (VE)-cadherin levels was observed in pirfenidone-treated Fra-2 TG mice. In contrast, eosinophil and VE-cadherin levels were unchanged in bleomycin-treated mice and not influenced by pirfenidone. In vitro, pirfenidone exacerbated the IL-4 induced reduction of endothelial barrier resistance, leading to higher leukocyte transmigration. Conclusion This study shows that antifibrotic properties of pirfenidone may be overruled by unwanted interactions with pre-injured endothelium in a setting of high T-helper type 2 inflammation in a model of SSc-ILD. Careful ILD patient phenotyping may be required to exploit benefits of pirfenidone while avoiding therapy failure and additional lung damage in some patients.

Original language	English
Article number	2102347
Journal	European Respiratory Journal
Volume	60
Issue number	4
DOIs	https://doi.org/10.1183/13993003.02347-2021
Publication status	Published - 01 Oct 2022
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

ASJC Scopus subject areas

Pulmonary and Respiratory Medicine

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10.1183/13993003.02347-2021

Cite this

Birnhuber, A., Jandl, K., Biasin, V., Fließer, E., Valzano, F., Marsh, L. M., Krolczik, C., Olschewski, A., Wilhelm, J., Toller, W., Heinemann, A., Olschewski, H., Wygrecka, M., & Kwapiszewska, G. (2022). Pirfenidone exacerbates Th2-driven vasculopathy in a mouse model of systemic sclerosis-associated interstitial lung disease. European Respiratory Journal, 60(4), Article 2102347. https://doi.org/10.1183/13993003.02347-2021

@article{5afe1c7dacb94bdb922263b0cd6d5d13,

title = "Pirfenidone exacerbates Th2-driven vasculopathy in a mouse model of systemic sclerosis-associated interstitial lung disease",

abstract = "Background Systemic sclerosis (SSc) is an autoimmune disease characterised by severe vasculopathy and fibrosis of various organs including the lung. Targeted treatment options for SSc-associated interstitial lung disease (SSc-ILD) are scarce. We assessed the effects of pirfenidone in a mouse model of SSc-ILD. Methods Pulmonary function, inflammation and collagen deposition in response to pirfenidone were assessed in Fra-2-overexpressing transgenic (Fra-2 TG) and bleomycin-treated mice. In Fra-2 TG mice, lung transcriptome was analysed after pirfenidone treatment. In vitro, pirfenidone effects on human eosinophil and endothelial cell function were analysed using flow cytometry-based assays and electric cell-substrate impedance measurements, respectively. Results Pirfenidone treatment attenuated pulmonary remodelling in the bleomycin model, but aggravated pulmonary inflammation, fibrosis and vascular remodelling in Fra-2 TG mice. Pirfenidone increased interleukin (IL)-4 levels and eosinophil numbers in lung tissue of Fra-2 TG mice without directly affecting eosinophil activation and migration in vitro. A pronounced immune response with high levels of cytokines/ chemokines and disturbed endothelial integrity with low vascular endothelial (VE)-cadherin levels was observed in pirfenidone-treated Fra-2 TG mice. In contrast, eosinophil and VE-cadherin levels were unchanged in bleomycin-treated mice and not influenced by pirfenidone. In vitro, pirfenidone exacerbated the IL-4 induced reduction of endothelial barrier resistance, leading to higher leukocyte transmigration. Conclusion This study shows that antifibrotic properties of pirfenidone may be overruled by unwanted interactions with pre-injured endothelium in a setting of high T-helper type 2 inflammation in a model of SSc-ILD. Careful ILD patient phenotyping may be required to exploit benefits of pirfenidone while avoiding therapy failure and additional lung damage in some patients.",

author = "Anna Birnhuber and Katharina Jandl and Valentina Biasin and Elisabeth Flie{\ss}er and Francesco Valzano and Marsh, \{Leigh M.\} and Christina Krolczik and Andrea Olschewski and Jochen Wilhelm and Wolfgang Toller and Akos Heinemann and Horst Olschewski and Malgorzata Wygrecka and Grazyna Kwapiszewska",

note = "Publisher Copyright: Copyright {\textcopyright}The authors 2022.",

year = "2022",

month = oct,

day = "1",

doi = "10.1183/13993003.02347-2021",

language = "English",

volume = "60",

journal = "European Respiratory Journal",

issn = "0903-1936",

publisher = "European Respiratory Society",

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Birnhuber, A, Jandl, K, Biasin, V, Fließer, E, Valzano, F, Marsh, LM, Krolczik, C, Olschewski, A, Wilhelm, J, Toller, W, Heinemann, A, Olschewski, H, Wygrecka, M & Kwapiszewska, G 2022, 'Pirfenidone exacerbates Th2-driven vasculopathy in a mouse model of systemic sclerosis-associated interstitial lung disease', European Respiratory Journal, vol. 60, no. 4, 2102347. https://doi.org/10.1183/13993003.02347-2021

TY - JOUR

T1 - Pirfenidone exacerbates Th2-driven vasculopathy in a mouse model of systemic sclerosis-associated interstitial lung disease

AU - Birnhuber, Anna

AU - Jandl, Katharina

AU - Biasin, Valentina

AU - Fließer, Elisabeth

AU - Valzano, Francesco

AU - Marsh, Leigh M.

AU - Krolczik, Christina

AU - Olschewski, Andrea

AU - Wilhelm, Jochen

AU - Toller, Wolfgang

AU - Heinemann, Akos

AU - Olschewski, Horst

AU - Wygrecka, Malgorzata

AU - Kwapiszewska, Grazyna

PY - 2022/10/1

Y1 - 2022/10/1

N2 - Background Systemic sclerosis (SSc) is an autoimmune disease characterised by severe vasculopathy and fibrosis of various organs including the lung. Targeted treatment options for SSc-associated interstitial lung disease (SSc-ILD) are scarce. We assessed the effects of pirfenidone in a mouse model of SSc-ILD. Methods Pulmonary function, inflammation and collagen deposition in response to pirfenidone were assessed in Fra-2-overexpressing transgenic (Fra-2 TG) and bleomycin-treated mice. In Fra-2 TG mice, lung transcriptome was analysed after pirfenidone treatment. In vitro, pirfenidone effects on human eosinophil and endothelial cell function were analysed using flow cytometry-based assays and electric cell-substrate impedance measurements, respectively. Results Pirfenidone treatment attenuated pulmonary remodelling in the bleomycin model, but aggravated pulmonary inflammation, fibrosis and vascular remodelling in Fra-2 TG mice. Pirfenidone increased interleukin (IL)-4 levels and eosinophil numbers in lung tissue of Fra-2 TG mice without directly affecting eosinophil activation and migration in vitro. A pronounced immune response with high levels of cytokines/ chemokines and disturbed endothelial integrity with low vascular endothelial (VE)-cadherin levels was observed in pirfenidone-treated Fra-2 TG mice. In contrast, eosinophil and VE-cadherin levels were unchanged in bleomycin-treated mice and not influenced by pirfenidone. In vitro, pirfenidone exacerbated the IL-4 induced reduction of endothelial barrier resistance, leading to higher leukocyte transmigration. Conclusion This study shows that antifibrotic properties of pirfenidone may be overruled by unwanted interactions with pre-injured endothelium in a setting of high T-helper type 2 inflammation in a model of SSc-ILD. Careful ILD patient phenotyping may be required to exploit benefits of pirfenidone while avoiding therapy failure and additional lung damage in some patients.

AB - Background Systemic sclerosis (SSc) is an autoimmune disease characterised by severe vasculopathy and fibrosis of various organs including the lung. Targeted treatment options for SSc-associated interstitial lung disease (SSc-ILD) are scarce. We assessed the effects of pirfenidone in a mouse model of SSc-ILD. Methods Pulmonary function, inflammation and collagen deposition in response to pirfenidone were assessed in Fra-2-overexpressing transgenic (Fra-2 TG) and bleomycin-treated mice. In Fra-2 TG mice, lung transcriptome was analysed after pirfenidone treatment. In vitro, pirfenidone effects on human eosinophil and endothelial cell function were analysed using flow cytometry-based assays and electric cell-substrate impedance measurements, respectively. Results Pirfenidone treatment attenuated pulmonary remodelling in the bleomycin model, but aggravated pulmonary inflammation, fibrosis and vascular remodelling in Fra-2 TG mice. Pirfenidone increased interleukin (IL)-4 levels and eosinophil numbers in lung tissue of Fra-2 TG mice without directly affecting eosinophil activation and migration in vitro. A pronounced immune response with high levels of cytokines/ chemokines and disturbed endothelial integrity with low vascular endothelial (VE)-cadherin levels was observed in pirfenidone-treated Fra-2 TG mice. In contrast, eosinophil and VE-cadherin levels were unchanged in bleomycin-treated mice and not influenced by pirfenidone. In vitro, pirfenidone exacerbated the IL-4 induced reduction of endothelial barrier resistance, leading to higher leukocyte transmigration. Conclusion This study shows that antifibrotic properties of pirfenidone may be overruled by unwanted interactions with pre-injured endothelium in a setting of high T-helper type 2 inflammation in a model of SSc-ILD. Careful ILD patient phenotyping may be required to exploit benefits of pirfenidone while avoiding therapy failure and additional lung damage in some patients.

UR - https://www.scopus.com/pages/publications/85133757518

U2 - 10.1183/13993003.02347-2021

DO - 10.1183/13993003.02347-2021

M3 - Journal article

C2 - 35332068

AN - SCOPUS:85133757518

SN - 0903-1936

VL - 60

JO - European Respiratory Journal

JF - European Respiratory Journal

IS - 4

M1 - 2102347

ER -

Pirfenidone exacerbates Th2-driven vasculopathy in a mouse model of systemic sclerosis-associated interstitial lung disease

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