Dopamine D1 receptor stimulates cathepsin K-dependent degradation and resorption of collagen I in lung fibroblasts

Matrix resorption is essential to the clearance of the extracellular matrix (ECM) after normal wound healing. A disruption in these processes constitutes a main component of fibrotic diseases, characterized by excess deposition and diminished clearance of fibrillar ECM proteins, such as collagen typ...

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Published inJournal of cell science Vol. 133; no. 23
Main Authors Diaz-Espinosa, Ana M, Link, Patrick A, Sicard, Delphine, Jorba, Ignasi, Tschumperlin, Daniel J, Haak, Andrew J
Format Journal Article
LanguageEnglish
Published England The Company of Biologists Ltd 11.12.2020
Subjects
Animals
Cathepsin K - genetics
Cells, Cultured
Collagen
Collagen Type I - genetics
Extracellular Matrix
Fibroblasts
Lung
Mice
Receptors, Dopamine D1 - genetics
Resorption
Cathepsin K
Dopamine receptor
Fibrosis
Resolution
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Summary:Matrix resorption is essential to the clearance of the extracellular matrix (ECM) after normal wound healing. A disruption in these processes constitutes a main component of fibrotic diseases, characterized by excess deposition and diminished clearance of fibrillar ECM proteins, such as collagen type I. The mechanisms and stimuli regulating ECM resorption in the lung remain poorly understood. Recently, agonism of dopamine receptor D1 (DRD1), which is predominantly expressed on fibroblasts in the lung, has been shown to accelerate tissue repair and clearance of ECM following bleomycin injury in mice. Therefore, we investigated whether DRD1 receptor signaling promotes the degradation of collagen type I by lung fibroblasts. For cultured fibroblasts, we found that DRD1 agonism enhances extracellular cleavage, internalization and lysosomal degradation of collagen I mediated by cathepsin K, which results in reduced stiffness of cell-derived matrices, as measured by atomic force microscopy. agonism of DRD1 similarly enhanced fibrillar collagen degradation by fibroblasts, as assessed by tissue labeling with a collagen-hybridizing peptide. Together, these results implicate DRD1 agonism in fibroblast-mediated collagen clearance, suggesting an important role for this mechanism in fibrosis resolution.This article has an associated First Person interview with the first author of the paper.
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Handling Editor: John Heath
ISSN:0021-9533
1477-9137
DOI:10.1242/jcs.248278