Mitochondrial catalase overexpressed transgenic mice are protected against lung fibrosis in part via preventing alveolar epithelial cell mitochondrial DNA damage

Seok-Jo Kim; Paul Cheresh; Renea P Jablonski; Luisa Morales-Nebreda; Yuan Cheng; Erin Hogan; Anjana Yeldandi; Monica Chi; Raul Piseaux; Karen Ridge; C Michael Hart; Navdeep Chandel; G R Scott Budinger; David W Kamp

doi:10.1016/j.freeradbiomed.2016.11.007

Mitochondrial catalase overexpressed transgenic mice are protected against lung fibrosis in part via preventing alveolar epithelial cell mitochondrial DNA damage

Free Radic Biol Med. 2016 Dec:101:482-490. doi: 10.1016/j.freeradbiomed.2016.11.007. Epub 2016 Nov 11.

Authors

Affiliations

¹ Department of Medicine, Division of Pulmonary & Critical Care Medicine, Jesse Brown VA Medical Center, Chicago, IL, United States; Department of Medicine, Northwestern University Feinberg School of Medicine, Chicago, IL 60611, United States.
² Department of Pathology, Northwestern University Feinberg School of Medicine, Chicago, IL 60611, United States.
³ Department of Medicine, Northwestern University Feinberg School of Medicine, Chicago, IL 60611, United States.
⁴ Atlanta VA Medical Center, Decatur, GA, United States; Department of Medicine, Emory University, Atlanta, GA, United States.
⁵ Department of Medicine, Division of Pulmonary & Critical Care Medicine, Jesse Brown VA Medical Center, Chicago, IL, United States; Department of Medicine, Northwestern University Feinberg School of Medicine, Chicago, IL 60611, United States. Electronic address: d-kamp@northwestern.edu.

PMID: 27840320
PMCID: PMC5928521
DOI: 10.1016/j.freeradbiomed.2016.11.007

Abstract

Rationale: Alveolar epithelial cell (AEC) injury and mitochondrial dysfunction are important in the development of lung fibrosis. Our group has shown that in the asbestos exposed lung, the generation of mitochondrial reactive oxygen species (ROS) in AEC mediate mitochondrial DNA (mtDNA) damage and apoptosis which are necessary for lung fibrosis. These data suggest that mitochondrial-targeted antioxidants should ameliorate asbestos-induced lung.

Objective: To determine whether transgenic mice that express mitochondrial-targeted catalase (MCAT) have reduced lung fibrosis following exposure to asbestos or bleomycin and, if so, whether this occurs in association with reduced AEC mtDNA damage and apoptosis.

Methods: Crocidolite asbestos (100µg/50µL), TiO₂ (negative control), bleomycin (0.025 units/50µL), or PBS was instilled intratracheally in 8-10 week-old wild-type (WT - C57Bl/6J) or MCAT mice. The lungs were harvested at 21d. Lung fibrosis was quantified by collagen levels (Sircol) and lung fibrosis scores. AEC apoptosis was assessed by cleaved caspase-3 (CC-3)/Surfactant protein C (SFTPC) immunohistochemistry (IHC) and semi-quantitative analysis. AEC (primary AT2 cells from WT and MCAT mice and MLE-12 cells) mtDNA damage was assessed by a quantitative PCR-based assay, apoptosis was assessed by DNA fragmentation, and ROS production was assessed by a Mito-Sox assay.

Results: Compared to WT, crocidolite-exposed MCAT mice exhibit reduced pulmonary fibrosis as measured by lung collagen levels and lung fibrosis score. The protective effects in MCAT mice were accompanied by reduced AEC mtDNA damage and apoptosis. Similar findings were noted following bleomycin exposure. Euk-134, a mitochondrial SOD/catalase mimetic, attenuated MLE-12 cell DNA damage and apoptosis. Finally, compared to WT, asbestos-induced MCAT AT2 cell ROS production was reduced.

Conclusions: Our finding that MCAT mice have reduced pulmonary fibrosis, AEC mtDNA damage and apoptosis following exposure to asbestos or bleomycin suggests an important role for AEC mitochondrial H₂O₂-induced mtDNA damage in promoting lung fibrosis. We reason that strategies aimed at limiting AEC mtDNA damage arising from excess mitochondrial H₂O₂ production may be a novel therapeutic target for mitigating pulmonary fibrosis.

Published by Elsevier Inc.

MeSH terms

Administration, Inhalation
Animals
Asbestos
Bleomycin
Caspase 3 / genetics
Caspase 3 / metabolism
Catalase / genetics*
Catalase / metabolism
Collagen / antagonists & inhibitors
Collagen / genetics
Collagen / metabolism
DNA, Mitochondrial / chemistry
DNA, Mitochondrial / drug effects*
DNA, Mitochondrial / metabolism
Epithelial Cells / drug effects*
Epithelial Cells / enzymology
Epithelial Cells / pathology
Gene Expression
Gene Expression Regulation
Intercellular Signaling Peptides and Proteins
Intubation, Intratracheal
Mice
Mice, Transgenic
Mitochondria / drug effects*
Mitochondria / enzymology
Mitochondria / pathology
Mitochondrial Proteins / genetics*
Mitochondrial Proteins / metabolism
Organometallic Compounds / pharmacology
Peptides / genetics
Peptides / metabolism
Pulmonary Alveoli / drug effects*
Pulmonary Alveoli / enzymology
Pulmonary Alveoli / pathology
Pulmonary Fibrosis / chemically induced
Pulmonary Fibrosis / genetics
Pulmonary Fibrosis / pathology
Pulmonary Fibrosis / prevention & control*
Pulmonary Surfactant-Associated Protein C
Reactive Oxygen Species / antagonists & inhibitors
Reactive Oxygen Species / metabolism
Salicylates / pharmacology
Transgenes

Substances

DNA, Mitochondrial
EUK-134
Intercellular Signaling Peptides and Proteins
Mitochondrial Proteins
Organometallic Compounds
Peptides
Pulmonary Surfactant-Associated Protein C
Reactive Oxygen Species
Salicylates
Sftpc protein, mouse
Bleomycin
Asbestos
Collagen
Catalase
Casp3 protein, mouse
Caspase 3

Abstract

MeSH terms

Substances

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