Fibrotic extracellular matrix activates a profibrotic positive feedback loop
Matthew W. Parker, … , Ola Larsson, Peter B. Bitterman
Matthew W. Parker, … , Ola Larsson, Peter B. Bitterman
Published March 3, 2014
Citation Information: J Clin Invest. 2014;124(4):1622-1635. https://doi.org/10.1172/JCI71386.
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Fibrotic extracellular matrix activates a profibrotic positive feedback loop

Abstract

Pathological remodeling of the extracellular matrix (ECM) by fibroblasts leads to organ failure. Development of idiopathic pulmonary fibrosis (IPF) is characterized by a progressive fibrotic scarring in the lung that ultimately leads to asphyxiation; however, the cascade of events that promote IPF are not well defined. Here, we examined how the interplay between the ECM and fibroblasts affects both the transcriptome and translatome by culturing primary fibroblasts generated from IPF patient lung tissue or nonfibrotic lung tissue on decellularized lung ECM from either IPF or control patients. Surprisingly, the origin of the ECM had a greater impact on gene expression than did cell origin, and differences in translational control were more prominent than alterations in transcriptional regulation. Strikingly, genes that were translationally activated by IPF-derived ECM were enriched for those encoding ECM proteins detected in IPF tissue. We determined that genes encoding IPF-associated ECM proteins are targets for miR-29, which was downregulated in fibroblasts grown on IPF-derived ECM, and baseline expression of ECM targets could be restored by overexpression of miR-29. Our data support a model in which fibroblasts are activated to pathologically remodel the ECM in IPF via a positive feedback loop between fibroblasts and aberrant ECM. Interrupting this loop may be a strategy for IPF treatment.

Authors

Matthew W. Parker, Daniel Rossi, Mark Peterson, Karen Smith, Kristina Sikström, Eric S. White, John E. Connett, Craig A. Henke, Ola Larsson, Peter B. Bitterman

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Figure 6

Overexpression of miR-29c abrogates pathological gene expression on IPF ECM.

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Overexpression of miR-29c abrogates pathological gene expression on IPF ...
(A) Experimental design of miR-29c function study. (B) Relative expression of miR-29c in IPF cells treated with miR-29c+ virus or with scrambled control virus. (C) Relative expression of four genes containing miR-29 targets quantified using qPCR from polysome-associated RNA. White bars represent samples treated with control virus. Black bars represent samples treated with miR-29+ virus. Data represent the mean ± SEM (three technical replicates). (D) Relative expression of four control genes. Controls were identified as genes that microarray indicated were upregulated by IPF but that did not contain miR-29 targets. (E) Relative expression of four ECM genes. ECM genes were identified as being upregulated by IPF but did not contain miR-29 targets.