Neutrophilic inflammation during lung development disrupts elastin assembly and predisposes adult mice to COPD
John T. Benjamin, Erin J. Plosa, Jennifer M.S. Sucre, Riet van der Meer, Shivangi Dave, Sergey Gutor, David S. Nichols, Peter M. Gulleman, Christopher S. Jetter, Wei Han, Matthew Xin, Peter C. Dinella, Ashley Catanzarite, Seunghyi Kook, Kalsang Dolma, Charitharth V. Lal, Amit Gaggar, J. Edwin Blalock, Dawn C. Newcomb, Bradley W. Richmond, Jonathan A. Kropski, Lisa R. Young, Susan H. Guttentag, Timothy S. Blackwell
John T. Benjamin, Erin J. Plosa, Jennifer M.S. Sucre, Riet van der Meer, Shivangi Dave, Sergey Gutor, David S. Nichols, Peter M. Gulleman, Christopher S. Jetter, Wei Han, Matthew Xin, Peter C. Dinella, Ashley Catanzarite, Seunghyi Kook, Kalsang Dolma, Charitharth V. Lal, Amit Gaggar, J. Edwin Blalock, Dawn C. Newcomb, Bradley W. Richmond, Jonathan A. Kropski, Lisa R. Young, Susan H. Guttentag, Timothy S. Blackwell
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Research Article Inflammation Pulmonology

Neutrophilic inflammation during lung development disrupts elastin assembly and predisposes adult mice to COPD

Abstract

Emerging evidence indicates that early life events can increase the risk for developing chronic obstructive pulmonary disease (COPD). Using an inducible transgenic mouse model for NF-κB activation in the airway epithelium, we found that a brief period of inflammation during the saccular stage (P3–P5) but not alveolar stage (P10–P12) of lung development disrupted elastic fiber assembly, resulting in permanent reduction in lung function and development of a COPD-like lung phenotype that progressed through 24 months of age. Neutrophil depletion prevented disruption of elastic fiber assembly and restored normal lung development. Mechanistic studies uncovered a role for neutrophil elastase (NE) in downregulating expression of critical elastic fiber assembly components, particularly fibulin-5 and elastin. Further, purified human NE and NE-containing exosomes from tracheal aspirates of premature infants with lung inflammation downregulated elastin and fibulin-5 expression by saccular-stage mouse lung fibroblasts. Together, our studies define a critical developmental window for assembling the elastin scaffold in the distal lung, which is required to support lung structure and function throughout the lifespan. Although neutrophils play a well-recognized role in COPD development in adults, neutrophilic inflammation may also contribute to early-life predisposition to COPD.

Authors

John T. Benjamin, Erin J. Plosa, Jennifer M.S. Sucre, Riet van der Meer, Shivangi Dave, Sergey Gutor, David S. Nichols, Peter M. Gulleman, Christopher S. Jetter, Wei Han, Matthew Xin, Peter C. Dinella, Ashley Catanzarite, Seunghyi Kook, Kalsang Dolma, Charitharth V. Lal, Amit Gaggar, J. Edwin Blalock, Dawn C. Newcomb, Bradley W. Richmond, Jonathan A. Kropski, Lisa R. Young, Susan H. Guttentag, Timothy S. Blackwell

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Figure 9

Neutrophil elastase downregulates TGF-β signaling and reduces elastin expression in saccular-stage lung fibroblasts.

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Neutrophil elastase downregulates TGF-β signaling and reduces elastin ex...
(A and B) P5 mouse lung fibroblasts were transfected with a Smad LUC reporter (SBE4-LUC) and treated with or without HNE (1 μg/mL) and/or recombinant TGF-β1 (0.1 ng/mL) for 12 hours. Luminescence measurements are reported as relative light units (RLU) above background (untransfected control) in (A) control cells and (B) TGF-β1–treated cells. Data are expressed as mean ± SEM, n = 4 per group. *P < 0.05 by 2-tailed Student’s t test. (CE) Mouse lung fibroblasts were cultured with or without HNE (1 μg/mL) and TGF-β1(0.1 ng/mL) for 24 hours. (C) mRNA expression of Ctgf, Serpine1, and Thbs1 in fibroblasts treated with or without HNE. Data are from 3 independent experiments and expressed as mean ± SEM, n = 7 per group. *P < 0.05 by 2-tailed Student’s t test. (D and E) mRNA expression of Eln (D) and Fbln5 (E) in saccular-stage fibroblasts treated with HNE ± recombinant TGF-β1. Data are from 3 independent experiments and expressed as mean ± SEM, n = 6–8 per group, *P < 0.05 compared with control by 1-way ANOVA and post hoc Tukey test.