Abstract
Metabolic reprogramming of the myofibroblast plays a fundamental role in the pathogenesis of fibrosing interstitial lung diseases. Here, we characterized the in vitro and in vivo metabolic and antifibrotic effects of IM156, an oxidative phosphorylation (OXPHOS) modulator that acts by inhibiting protein complex 1. In vitro, IM156 inhibited transforming growth factor β (TGFβ)-dependent increases in mitochondrial oxygen consumption rate and expression of myofibroblast markers in human pulmonary fibroblasts without altering cell viability or adding to TGFβ-induced increases in the extracellular acidification rate. IM156 significantly increased cellular AMP-activated protein kinase (AMPK) phosphorylation and was 60-fold more potent than metformin. In vivo, chronic oral administration of IM156 was highly distributed to major peripheral organs (i.e., lung, liver, kidney, heart) and had significant dose-related effects on the plasma metabolome consistent with OXPHOS modulation and AMPK activation. IM156 increased glycolysis, lipolysis, β-oxidation, and amino acids and decreased free fatty acids, tricarboxylic acid cycle activity, and protein synthesis. In the murine bleomycin model of pulmonary fibrosis, daily oral administration of IM156, administered 7 days after lung injury, attenuated body/lung weight changes and reduced lung fibrosis and inflammatory cell infiltration. The plasma exposures of IM156 were comparable to well tolerated doses in human studies. In conclusion, the metabolic and antifibrotic effects of IM156 suggest that OXPHOS modulation can attenuate myofibroblast metabolic reprogramming and support testing IM156 as a therapy for idiopathic pulmonary fibrosis and other fibrotic diseases. SIGNIFICANCE STATEMENT: Fibrosing interstitial lung diseases have a poor prognosis, and current antifibrotic treatments have significant limitations. This study demonstrates that attenuation of fibrogenic metabolic remodeling, by modulation of oxidative phosphorylation with IM156, prevents myofibroblast phenotype/collagen deposition and is a potentially effective and translational antifibrotic strategy.
Highlights
Progressive tissue fibrosis is associated with poor patient outcomes and high health care costs in a wide variety of rare and common diseases (Zhao et al, 2020), including fibrosing interstitial lung diseases (FILDs), of which idiopathic pulmonary fibrosis (IPF) is the best characterized (Kolb and Vasakova, 2019)
In the present study we have focused on the role of oxidative phosphorylation (OXPHOS) in the myofibroblast phenotype, metabolism, and fibrosis by evaluating the in vitro and in vivo effects of IM156, a selective mitochondrial protein complex 1 (PC1) modulator (Izreig et al, 2020)
IM156 abolished the effects of transforming growth factor b (TGFb) on oxygen consumption rate (OCR) (Fig. 1, A and B), and the effects of IM156 and TGF on extracellular acidification rate (ECAR) were not additive (Fig. 1, C, D, and F)
Summary
Progressive tissue fibrosis is associated with poor patient outcomes and high health care costs in a wide variety of rare and common diseases (Zhao et al, 2020), including fibrosing interstitial lung diseases (FILDs), of which idiopathic pulmonary fibrosis (IPF) is the best characterized (Kolb and Vasakova, 2019). Critical to ABBREVIATIONS: A.A, antibiotic-antimycotic; AMPK, AMP-activated protein kinase; BAL, bronchioalveolar lavage; COL1A1, type-1 collagen; ECAR, extracellular acidification rate; EMEM, Eagle’s minimum essential medium; FILD, fibrosing interstitial lung disease; IPF, idiopathic pulmonary fibrosis; LC-MS/MS, liquid chromatography–tandem mass spectrometry; MT, Masson’s trichrome; OCR, oxygen consumption rate; OXPHOS, oxidative phosphorylation; PC1, protein complex 1; a-SMA, a-smooth muscle actin; TCA, tricarboxylic acid; TFI, total fluorescence intensity; TGFb, transforming growth factor b
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