Microarray profiling reveals suppressed interferon stimulated gene program in fibroblasts from scleroderma-associated interstitial lung disease
Gisela E. Lindahl,Carmel Stock,Xu Shiwen,Patricia Leoni,Piersante Sestini,Sarah L. Howat,George Bou-Gharios,Andrew G. Nicholson,Christopher P. Denton,Jan C. Grutters,Toby M. Maher,Athol U. Wells,David Abraham,Elisabetta A. Renzoni +13 more
TL;DR: The data suggests that the repressed expression of interferon-stimulated genes may underpin critical aspects of the profibrotic fibroblast phenotype, identifying an area in pulmonary fibrosis that requires further investigation.
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Abstract: Interstitial lung disease is a major cause of morbidity and mortality in systemic sclerosis (SSc), with insufficiently effective treatment options. Progression of pulmonary fibrosis involves expanding populations of fibroblasts, and the accumulation of extracellular matrix proteins. Characterisation of SSc lung fibroblast gene expression profiles underlying the fibrotic cell phenotype could enable a better understanding of the processes leading to the progressive build-up of scar tissue in the lungs. In this study we evaluate the transcriptomes of fibroblasts isolated from SSc lung biopsies at the time of diagnosis, compared with those from control lungs. We used Affymetrix oligonucleotide microarrays to compare the gene expression profile of pulmonary fibroblasts cultured from 8 patients with pulmonary fibrosis associated with SSc (SSc-ILD), with those from control lung tissue peripheral to resected cancer (n=10). Fibroblast cultures from 3 patients with idiopathic pulmonary fibrosis (IPF) were included as a further comparison. Genes differentially expressed were identified using two separate analysis programs following a set of pre-determined criteria: only genes significant in both analyses were considered. Microarray expression data was verified by qRT-PCR and/or western blot analysis. A total of 843 genes were identified as differentially expressed in pulmonary fibroblasts from SSc-ILD and/or IPF compared to control lung, with a large overlap in the expression profiles of both diseases. We observed increased expression of a TGF-β response signature including fibrosis associated genes and myofibroblast markers, with marked heterogeneity across samples. Strongly suppressed expression of interferon stimulated genes, including antiviral, chemokine, and MHC class 1 genes, was uniformly observed in fibrotic fibroblasts. This expression profile includes key regulators and mediators of the interferon response, such as STAT1, and CXCL10, and was also independent of disease group. This study identified a strongly suppressed interferon-stimulated gene program in fibroblasts from fibrotic lung. The data suggests that the repressed expression of interferon-stimulated genes may underpin critical aspects of the profibrotic fibroblast phenotype, identifying an area in pulmonary fibrosis that requires further investigation.
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Citations
IL-11 is a crucial determinant of cardiovascular fibrosis
Sebastian Schafer,Sivakumar Viswanathan,Anissa A. Widjaja,W. Lim,Aida Moreno-Moral,Daniel M. DeLaughter,Benjamin Ng,Giannino Patone,Kingsley Chow,Ester Khin,Jessie Tan,Sonia Chothani,Lei Ye,Owen J. L. Rackham,Nicole S. J. Ko,Norliza E Sahib,Chee Jian Pua,Nicole T G Zhen,Chen Xie,Mao Wang,Henrike Maatz,Shiqi Lim,Kathrin Saar,Susanne Blachut,Enrico Petretto,Sabine Schmidt,Tracy L Putoczki,Tracy L Putoczki,Nuno Guimarães-Camboa,Hiroko Wakimoto,Sebastiaan van Heesch,Kristmundur Sigmundsson,See L Lim,Jia L Soon,Victor Tt Chao,Yeow L Chua,Teing Ee Tan,Sylvia M. Evans,Sylvia M. Evans,Yee J Loh,Muhammad H. Jamal,Kim K Ong,Kim C. Chua,Boon-Hean Ong,Mathew J Chakaramakkil,Jonathan G. Seidman,Christine E. Seidman,Christine E. Seidman,Christine E. Seidman,Norbert Hubner,Kenny Yk Sin,Stuart A. Cook +51 more
TL;DR: It is shown that upregulation of interleukin-11 (IL-11) is the dominant transcriptional response to TGFβ1 exposure and required for its pro-fibrotic effect, and proposed that inhibition of IL-11 is a potential therapeutic strategy to treat fibrotic diseases.
Interleukin-11 is a therapeutic target in idiopathic pulmonary fibrosis.
Benjamin Ng,Jinrui Dong,Giuseppe D'Agostino,Sivakumar Viswanathan,Anissa A. Widjaja,W. Lim,Nicole S. J. Ko,Jessie Tan,Sonia Chothani,Benjamin Huang,Chen Xie,Chee Jian Pua,Ann-Marie Chacko,Nuno Guimarães-Camboa,Nuno Guimarães-Camboa,Sylvia M. Evans,Sylvia M. Evans,Adam J. Byrne,Toby M. Maher,Jiurong Liang,Dianhua Jiang,Paul W. Noble,Sebastian Schafer,Stuart A. Cook +23 more
TL;DR: It is shown that interleukin-11 (IL11) is up-regulated in the lung of patients with IPF, associated with disease severity, and IL-11 is secreted from IPF fibroblasts, and these data prioritize IL- 11 as a drug target for lung fibrosis and IPF.
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Interstitial lung disease
Katerina M. Antoniou,George A. Margaritopoulos,George A. Margaritopoulos,S. Tomassetti,S. Tomassetti,Francesco Bonella,Francesco Bonella,Ulrich Costabel,Ulrich Costabel,Venerino Poletti,Venerino Poletti +10 more
TL;DR: This work has shown that biomarkers have been proposed in order to predict the course of the disease and group patients with the same characteristics in clinical trials and early diagnosis and disease stratification is important in the field of other interstitial lung diseases.
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Review: Interstitial Lung Disease Associated With Systemic Sclerosis and Idiopathic Pulmonary Fibrosis: How Similar and Distinct?
Erica L. Herzog,Aditi Mathur,Andrew M. Tager,Carol Feghali-Bostwick,Frank Schneider,John Varga +5 more
TL;DR: This review compares and contrasts salient features of SSc-associated interstitial lung disease and idiopathic pulmonary fibrosis, focusing on clinical manifestations, lung imaging, and pathology, along with current concepts of pathogenesis, including animal models, translational studies, genetic factors, and predictive biomarkers.
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Role of JAK/STAT in Interstitial Lung Diseases; Molecular and Cellular Mechanisms.
TL;DR: The JAK/STAT molecular pathway is activated under the interaction of a broad number of profibrotic/pro-inflammatory cytokines, such as IL-6, IL-11, and IL-13, which are increased in different ILDs as discussed by the authors.
164
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