CCR10+ epithelial cells from idiopathic pulmonary fibrosis lungs drive remodeling
David M. Habiel, Milena S. Espindola, Isabelle C. Jones, Ana Lucia Coelho, Barry Stripp, Cory M. Hogaboam
David M. Habiel, Milena S. Espindola, Isabelle C. Jones, Ana Lucia Coelho, Barry Stripp, Cory M. Hogaboam
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Research Article Cell biology Pulmonology

CCR10+ epithelial cells from idiopathic pulmonary fibrosis lungs drive remodeling

Abstract

Idiopathic pulmonary fibrosis (IPF) is a devastating fibrotic lung disease of unknown etiology and limited therapeutic options. In this report, we characterize what we believe is a novel CCR10+ epithelial cell population in IPF lungs. There was a significant increase in the percentage of CCR10+ epithelial cells in IPF relative to normal lung explants and their numbers significantly correlated to lung remodeling in humanized NSG mice. Cultured CCR10-enriched IPF epithelial cells promoted IPF lung fibroblast invasion and collagen 1 secretion. Single-cell RNA sequencing analysis showed distinct CCR10+ epithelial cell populations enriched for inflammatory and profibrotic transcripts. Consistently, cultured IPF but not normal epithelial cells induced lung remodeling in humanized NSG mice, where the number of CCR10+ IPF, but not normal, epithelial cells correlated with hydroxyproline concentration in the remodeled NSG lungs. A subset of IPF CCR10hi epithelial cells coexpress EphA3 and ephrin A signaling induces the expression of CCR10 by these cells. Finally, EphA3+CCR10hi epithelial cells induce more consistent lung remodeling in NSG mice relative to EphA3–CCR10lo epithelial cells. Our results suggest that targeting epithelial cells, highly expressing CCR10, may be beneficial in IPF.

Authors

David M. Habiel, Milena S. Espindola, Isabelle C. Jones, Ana Lucia Coelho, Barry Stripp, Cory M. Hogaboam

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Figure 9

CCR10+EphA3+ epithelial cells induce consistent lung remodeling in NSG mice.

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CCR10+EphA3+ epithelial cells induce consistent lung remodeling in NSG m...
(A) Magnetic sorting of EphA3+ and EphA3 IPF explant cells, followed by expansion of epithelial cells via CRC culture and subsequent i.v. administration into NSG mice. (B and C) Shown are images of CRC-expanded EphA3 (B) and EphA3+ (C) epithelial cells acquired at ×100 magnification. (D and E) Masson’s trichrome staining of NSG lungs 63 days after EphA3 (D) or EphA3+ (E) epithelial cell administration. (F) Depicted is the average hydroxyproline concentration in lungs tissues from naive or humanized NSG mice. Naive: n = 4; IPF CRC: n = 5/group. *P ≤ 0.05 via 1-way ANOVA corrected with Dunnett’s test. (G) Shown are representative dot plots depicting IPF xenografted EpCAM+ epithelial cells (top) staining for CCR10 (middle) and EphA3 (bottom) proteins in IPF EphA3 (left) or EphA3+ (right) epithelial cell–humanized NSG lungs. (H and I) Shown is the percentage of CD45EpCAM+CCR10+EphA3+ (H) and CCR10 GMFI of CD45EpCAM+ cells in the lungs of mice humanized with EphA3 or EphA3+ IPF epithelial cells. Data shown are the mean± SEM.; n = 5/group. *P ≤ 0.05; **P ≤ 0.01 via unpaired Mann-Whitney 2-tailed nonparametric test. IPF, idiopathic pulmonary fibrosis; CRC, conditionally reprogrammed cell culture medium; NSG, NOD Cg-PrkdcSCID IL2rgTm1wilSzi.