Circulating monocytes from systemic sclerosis patients with interstitial lung disease show an enhanced profibrotic phenotype

Susan K. Mathai; Mridu Gulati; Xueyan Peng; Thomas R. Russell; Albert C. Shaw; Ami N. Rubinowitz; Lynne A. Murray; Jonathan M. Siner; Danielle E. Antin-Ozerkis; Ruth R. Montgomery; Ronald As Reilkoff; Richard J. Bucala; Erica L. Herzog

doi:10.1038/labinvest.2010.73

Circulating monocytes from systemic sclerosis patients with interstitial lung disease show an enhanced profibrotic phenotype

Susan K. Mathai, Mridu Gulati, Xueyan Peng, Thomas R. Russell, Albert C. Shaw, Ami N. Rubinowitz, Lynne A. Murray, Jonathan M. Siner, Danielle E. Antin-Ozerkis, Ruth R. Montgomery, Ronald As Reilkoff, Richard J. Bucala, Erica L. Herzog

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187 Scopus citations

Abstract

Profibrotic cells derived from circulating CD14+ monocytes include fibrocytes and alternatively activated macrophages. These cells are associated with interstitial lung disease (ILD) and are implicated in the pathogenesis of systemic sclerosis (SSc); however, the simultaneous presence of profibrotic cells and their associated mediators in the circulation of these patients has not been defined. We hypothesized that monocytes from patients with SSc-related ILD (SSc-ILD) would show profibrotic characteristics when compared with normal controls. We recruited patients with SSc-ILD (n=12) and normal controls (n=27) and quantified circulating collagen-producing cells by flow cytometry for CD45 and pro-collagen I. The in vitro activation potential of CD14+ monocytes in response to lipopolysaccharide was assessed using flow cytometry for CD163, and by ELISA for CCL18 and IL-10 secretion. Profibrotic mediators in plasma were quantified using Luminexbased assays. The concentration of circulating collagen-producing cells was increased in the SSc-ILD patients when compared with controls. These cells were composed of both CD34+ fibrocytes and a population of CD34+CD14+ cells. Cultured CD14+ monocytes from SSc-ILD patients revealed a profibrotic phenotype characterized by expression of CD163 and by enhanced secretion of CCL18 and IL-10 in response to proinflammatory activation. Plasma levels of IL-10, MCP-1, IL-1RA, and TNF levels were significantly elevated in the plasma of the SSc-ILD cohort. Subgroup analysis of the normal controls revealed that unlike the subjects ≤35 years, subjects ≥60 years old showed higher levels of circulating CD34+CD14+ cells, collagen-producing CD14+ monocytes, CD163+ monocytes, IL-4, IL-10, IL-13, MCP-1, and CCL18. These data indicate that the blood of patients with SSc-ILD and of healthy aged controls is enriched for fibrocytes, profibrotic monocytes, and fibrosis-associated mediators. Investigations defining the factors responsible for this peripheral blood profile may provide new insight into SSc-ILD as well as the pathophysiology of aging.

Original language	English (US)
Pages (from-to)	812-823
Number of pages	12
Journal	Laboratory Investigation
Volume	90
Issue number	6
DOIs	https://doi.org/10.1038/labinvest.2010.73
State	Published - Jun 2010
Externally published	Yes

Bibliographical note

Funding Information:
This work was supported in part by awards from the NIH (P30AR053495-01A1, K08 HL079066, UL1 RR024139, and N01 A150031) an Edward Mallinckrodt, Jr Scholar Award, funds from the Yale Department of Medicine, and Promedior, Inc. (all to ELH).

Keywords

Alternative activation
Fibrocytes
Macrophages
Pulmonary fibrosis
Scleroderma

UN SDGs

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

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Mathai, S. K., Gulati, M., Peng, X., Russell, T. R., Shaw, A. C., Rubinowitz, A. N., Murray, L. A., Siner, J. M., Antin-Ozerkis, D. E., Montgomery, R. R., Reilkoff, R. A., Bucala, R. J., & Herzog, E. L. (2010). Circulating monocytes from systemic sclerosis patients with interstitial lung disease show an enhanced profibrotic phenotype. Laboratory Investigation, 90(6), 812-823. https://doi.org/10.1038/labinvest.2010.73

Mathai, SK, Gulati, M, Peng, X, Russell, TR, Shaw, AC, Rubinowitz, AN, Murray, LA, Siner, JM, Antin-Ozerkis, DE, Montgomery, RR, Reilkoff, RA, Bucala, RJ & Herzog, EL 2010, 'Circulating monocytes from systemic sclerosis patients with interstitial lung disease show an enhanced profibrotic phenotype', Laboratory Investigation, vol. 90, no. 6, pp. 812-823. https://doi.org/10.1038/labinvest.2010.73

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title = "Circulating monocytes from systemic sclerosis patients with interstitial lung disease show an enhanced profibrotic phenotype",

abstract = "Profibrotic cells derived from circulating CD14+ monocytes include fibrocytes and alternatively activated macrophages. These cells are associated with interstitial lung disease (ILD) and are implicated in the pathogenesis of systemic sclerosis (SSc); however, the simultaneous presence of profibrotic cells and their associated mediators in the circulation of these patients has not been defined. We hypothesized that monocytes from patients with SSc-related ILD (SSc-ILD) would show profibrotic characteristics when compared with normal controls. We recruited patients with SSc-ILD (n=12) and normal controls (n=27) and quantified circulating collagen-producing cells by flow cytometry for CD45 and pro-collagen I. The in vitro activation potential of CD14+ monocytes in response to lipopolysaccharide was assessed using flow cytometry for CD163, and by ELISA for CCL18 and IL-10 secretion. Profibrotic mediators in plasma were quantified using Luminexbased assays. The concentration of circulating collagen-producing cells was increased in the SSc-ILD patients when compared with controls. These cells were composed of both CD34+ fibrocytes and a population of CD34+CD14+ cells. Cultured CD14+ monocytes from SSc-ILD patients revealed a profibrotic phenotype characterized by expression of CD163 and by enhanced secretion of CCL18 and IL-10 in response to proinflammatory activation. Plasma levels of IL-10, MCP-1, IL-1RA, and TNF levels were significantly elevated in the plasma of the SSc-ILD cohort. Subgroup analysis of the normal controls revealed that unlike the subjects ≤35 years, subjects ≥60 years old showed higher levels of circulating CD34+CD14+ cells, collagen-producing CD14+ monocytes, CD163+ monocytes, IL-4, IL-10, IL-13, MCP-1, and CCL18. These data indicate that the blood of patients with SSc-ILD and of healthy aged controls is enriched for fibrocytes, profibrotic monocytes, and fibrosis-associated mediators. Investigations defining the factors responsible for this peripheral blood profile may provide new insight into SSc-ILD as well as the pathophysiology of aging.",

keywords = "Alternative activation, Fibrocytes, Macrophages, Pulmonary fibrosis, Scleroderma",

author = "Mathai, {Susan K.} and Mridu Gulati and Xueyan Peng and Russell, {Thomas R.} and Shaw, {Albert C.} and Rubinowitz, {Ami N.} and Murray, {Lynne A.} and Siner, {Jonathan M.} and Antin-Ozerkis, {Danielle E.} and Montgomery, {Ruth R.} and Reilkoff, {Ronald As} and Bucala, {Richard J.} and Herzog, {Erica L.}",

note = "Funding Information: This work was supported in part by awards from the NIH (P30AR053495-01A1, K08 HL079066, UL1 RR024139, and N01 A150031) an Edward Mallinckrodt, Jr Scholar Award, funds from the Yale Department of Medicine, and Promedior, Inc. (all to ELH).",

year = "2010",

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doi = "10.1038/labinvest.2010.73",

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T1 - Circulating monocytes from systemic sclerosis patients with interstitial lung disease show an enhanced profibrotic phenotype

AU - Mathai, Susan K.

AU - Gulati, Mridu

AU - Peng, Xueyan

AU - Russell, Thomas R.

AU - Shaw, Albert C.

AU - Rubinowitz, Ami N.

AU - Murray, Lynne A.

AU - Siner, Jonathan M.

AU - Antin-Ozerkis, Danielle E.

AU - Montgomery, Ruth R.

AU - Reilkoff, Ronald As

AU - Bucala, Richard J.

AU - Herzog, Erica L.

N1 - Funding Information: This work was supported in part by awards from the NIH (P30AR053495-01A1, K08 HL079066, UL1 RR024139, and N01 A150031) an Edward Mallinckrodt, Jr Scholar Award, funds from the Yale Department of Medicine, and Promedior, Inc. (all to ELH).

PY - 2010/6

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N2 - Profibrotic cells derived from circulating CD14+ monocytes include fibrocytes and alternatively activated macrophages. These cells are associated with interstitial lung disease (ILD) and are implicated in the pathogenesis of systemic sclerosis (SSc); however, the simultaneous presence of profibrotic cells and their associated mediators in the circulation of these patients has not been defined. We hypothesized that monocytes from patients with SSc-related ILD (SSc-ILD) would show profibrotic characteristics when compared with normal controls. We recruited patients with SSc-ILD (n=12) and normal controls (n=27) and quantified circulating collagen-producing cells by flow cytometry for CD45 and pro-collagen I. The in vitro activation potential of CD14+ monocytes in response to lipopolysaccharide was assessed using flow cytometry for CD163, and by ELISA for CCL18 and IL-10 secretion. Profibrotic mediators in plasma were quantified using Luminexbased assays. The concentration of circulating collagen-producing cells was increased in the SSc-ILD patients when compared with controls. These cells were composed of both CD34+ fibrocytes and a population of CD34+CD14+ cells. Cultured CD14+ monocytes from SSc-ILD patients revealed a profibrotic phenotype characterized by expression of CD163 and by enhanced secretion of CCL18 and IL-10 in response to proinflammatory activation. Plasma levels of IL-10, MCP-1, IL-1RA, and TNF levels were significantly elevated in the plasma of the SSc-ILD cohort. Subgroup analysis of the normal controls revealed that unlike the subjects ≤35 years, subjects ≥60 years old showed higher levels of circulating CD34+CD14+ cells, collagen-producing CD14+ monocytes, CD163+ monocytes, IL-4, IL-10, IL-13, MCP-1, and CCL18. These data indicate that the blood of patients with SSc-ILD and of healthy aged controls is enriched for fibrocytes, profibrotic monocytes, and fibrosis-associated mediators. Investigations defining the factors responsible for this peripheral blood profile may provide new insight into SSc-ILD as well as the pathophysiology of aging.

AB - Profibrotic cells derived from circulating CD14+ monocytes include fibrocytes and alternatively activated macrophages. These cells are associated with interstitial lung disease (ILD) and are implicated in the pathogenesis of systemic sclerosis (SSc); however, the simultaneous presence of profibrotic cells and their associated mediators in the circulation of these patients has not been defined. We hypothesized that monocytes from patients with SSc-related ILD (SSc-ILD) would show profibrotic characteristics when compared with normal controls. We recruited patients with SSc-ILD (n=12) and normal controls (n=27) and quantified circulating collagen-producing cells by flow cytometry for CD45 and pro-collagen I. The in vitro activation potential of CD14+ monocytes in response to lipopolysaccharide was assessed using flow cytometry for CD163, and by ELISA for CCL18 and IL-10 secretion. Profibrotic mediators in plasma were quantified using Luminexbased assays. The concentration of circulating collagen-producing cells was increased in the SSc-ILD patients when compared with controls. These cells were composed of both CD34+ fibrocytes and a population of CD34+CD14+ cells. Cultured CD14+ monocytes from SSc-ILD patients revealed a profibrotic phenotype characterized by expression of CD163 and by enhanced secretion of CCL18 and IL-10 in response to proinflammatory activation. Plasma levels of IL-10, MCP-1, IL-1RA, and TNF levels were significantly elevated in the plasma of the SSc-ILD cohort. Subgroup analysis of the normal controls revealed that unlike the subjects ≤35 years, subjects ≥60 years old showed higher levels of circulating CD34+CD14+ cells, collagen-producing CD14+ monocytes, CD163+ monocytes, IL-4, IL-10, IL-13, MCP-1, and CCL18. These data indicate that the blood of patients with SSc-ILD and of healthy aged controls is enriched for fibrocytes, profibrotic monocytes, and fibrosis-associated mediators. Investigations defining the factors responsible for this peripheral blood profile may provide new insight into SSc-ILD as well as the pathophysiology of aging.

KW - Alternative activation

KW - Fibrocytes

KW - Macrophages

KW - Pulmonary fibrosis

KW - Scleroderma

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Circulating monocytes from systemic sclerosis patients with interstitial lung disease show an enhanced profibrotic phenotype

Abstract

Bibliographical note

Keywords

UN SDGs

Access

OpenUrl availability

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