Fibrocytes develop outside the kidney but contribute to renal fibrosis in a mouse model

Collagen-producing bone marrow–derived cells (fibrocytes) have been detected in animal models and patients with fibrotic diseases. In vitro data suggest that they develop from monocytes with the help of accessory cells and profibrotic soluble factors. Using a mouse model of renal fibrosis, unilatera...

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Published inKidney international Vol. 84; no. 1; pp. 78 - 89
Main Authors Reich, Barbara, Schmidbauer, Kathrin, Rodriguez Gomez, Manuel, Johannes Hermann, Fabian, Göbel, Nicole, Brühl, Hilke, Ketelsen, Isabel, Talke, Yvonne, Mack, Matthias
Format Journal Article
LanguageEnglish
Published United States Elsevier Inc 01.07.2013
Elsevier Limited
Subjects
Animals
Antigens, Ly - metabolism
Biomarkers - metabolism
CD11b Antigen - metabolism
cell ablation
Cell Differentiation
chemokine receptor
Chemotaxis
Collagen - metabolism
Disease Models, Animal
Female
Fibrosis
immunology
Kidney - metabolism
Kidney - pathology
Kidney Diseases - etiology
Kidney Diseases - genetics
Kidney Diseases - metabolism
Kidney Diseases - pathology
Mice
Mice, Inbred C57BL
Mice, Knockout
Monocytes - metabolism
Monocytes - pathology
Phenotype
Receptors, CCR2 - deficiency
Receptors, CCR2 - genetics
Time Factors
Ureteral Obstruction - complications
fibrosis
cell ablation
immunology
chemokine receptor
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Summary:Collagen-producing bone marrow–derived cells (fibrocytes) have been detected in animal models and patients with fibrotic diseases. In vitro data suggest that they develop from monocytes with the help of accessory cells and profibrotic soluble factors. Using a mouse model of renal fibrosis, unilateral ureteral obstruction, we found the number of circulating fibrocytes was not reduced when monocytes were depleted with a monoclonal antibody against CCR2 or when CCR2-/- mice with very low numbers of circulating or splenic monocytes were analyzed. The absence of CCR2, however, interfered with migration of fibrocytes into the kidney. The phenotype of splenic and renal fibrocytes was very similar and distinct from classical monocytes as fibrocytes expressed no CD115, medium levels of CCR2, and high levels of CD11b and Ly-6G. Using a depleting monoclonal antibody against Ly-6G or bone marrow chimeric mice expressing the diphtheria toxin receptor under the control of CD11b, we could efficiently deplete fibrocytes from the kidney. Depletion of fibrocytes or reduced migration of fibrocytes into the kidney resulted in lower renal expression of collagen-I. Thus, fibrocytes develop outside the kidney independent of infiltrating monocytes and rely on CCR2 for migration into target organs.
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ISSN:0085-2538
1523-1755
DOI:10.1038/ki.2013.84