CFTR Correctors and Antioxidants Partially Normalize Lipid Imbalance but not Abnormal Basal Inflammatory Cytokine Profile in CF Bronchial Epithelial Cells

Mieke Veltman, JB De Sanctis, Marta Stolarczyk, N Klymiuk, A Bahr, Rutger Brouwer, Edwin Oole, J Shah, T Ozdian, J Liao, C Martini, D Radzioch, JW Hanrahan, Bob Scholte

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Abstract

A deficiency in cystic fibrosis transmembrane conductance regulator (CFTR) function in CF leads to chronic lung disease. CF is associated with abnormalities in fatty acids, ceramides, and cholesterol, their relationship with CF lung pathology is not completely understood. Therefore, we examined the impact of CFTR deficiency on lipid metabolism and pro-inflammatory signaling in airway epithelium using mass spectrometric, protein array. We observed a striking imbalance in fatty acid and ceramide metabolism, associated with chronic oxidative stress under basal conditions in CF mouse lung and well-differentiated bronchial epithelial cell cultures of CFTR knock out pig and CF patients. Cell-autonomous features of all three CF models included high ratios of ω-6- to ω-3-polyunsaturated fatty acids and of long- to very long-chain ceramide species (LCC/VLCC), reduced levels of total ceramides and ceramide precursors. In addition to the retinoic acid analog fenretinide, the anti-oxidants glutathione (GSH) and deferoxamine partially corrected the lipid profile indicating that oxidative stress may promote the lipid abnormalities. CFTR-targeted modulators reduced the lipid imbalance and oxidative stress, confirming the CFTR dependence of lipid ratios. However, despite functional correction of CF cells up to 60% of non-CF in Ussing chamber experiments, a 72-h triple compound treatment (elexacaftor/tezacaftor/ivacaftor surrogate) did not completely normalize lipid imbalance or oxidative stress. Protein array analysis revealed differential expression and shedding of cytokines and growth factors from CF epithelial cells compared to non-CF cells, consistent with sterile inflammation and tissue remodeling under basal conditions, including enhanced secretion of the neutrophil activator CXCL5, and the T-cell activator CCL17. However, treatment with antioxidants or CFTR modulators that mimic the approved combination therapies, ivacaftor/lumacaftor and ivacaftor/tezacaftor/elexacaftor, did not effectively suppress the inflammatory phenotype. We propose that CFTR deficiency causes oxidative stress in CF airway epithelium, affecting multiple bioactive lipid metabolic pathways, which likely play a role in CF lung disease progression. A combination of anti-oxidant, anti-inflammatory and CFTR targeted therapeutics may be required for full correction of the CF phenotype.

Original languageEnglish
Article number619442
JournalFrontiers in Physiology
Volume12
DOIs
Publication statusPublished - 4 Feb 2021

Bibliographical note

Funding Information:
BS, MV, and MS were supported by EU ZONMW ERARE INSTINCT, Sophia Fund S19-06 WO, Longfonds 3.3.10.027, NCFS HITCF-7. JH was supported by grants HANRAH19G0 from the CFF (United States) and the E-Rare program funded by CF Canada, Fonds de recherche du Québec – Santé, and the Canadian Institutes of Health Research. ENOCH Molecular, cellular and clinical approach to healthy aging grant ENOCH; Registration Number: CZ.02.1.01/0.0/0.0/16_019/ 0000868 (JBS, DR, and TO).

Funding Information:
We thank the ERARE INSTINCT team at Hannover Germany for providing lung tissue, specifically Drs. Peter Braubach and Martin Ulrich (PI). Dr. Braubach is at the Arbeitsgruppe Lungenforschung, Institut f?r Pathologie Medizinische Hochschule Hannover OE 5110, Carl-Neuberg-Str. 1, 30625 Hannover, Deutschland. Funding. BS, MV, and MS were supported by EU ZONMW ERARE INSTINCT, Sophia Fund S19-06 WO, Longfonds 3.3.10.027, NCFS HITCF-7. JH was supported by grants HANRAH19G0 from the CFF (United States) and the E-Rare program funded by CF Canada, Fonds de recherche du Qu?bec ? Sant?, and the Canadian Institutes of Health Research. ENOCH Molecular, cellular and clinical approach to healthy aging grant ENOCH; Registration Number: CZ.02.1.01/0.0/0.0/16_019/ 0000868 (JBS, DR, and TO).

Publisher Copyright:
© Copyright © 2021 Veltman, De Sanctis, Stolarczyk, Klymiuk, Bähr, Brouwer, Oole, Shah, Ozdian, Liao, Martini, Radzioch, Hanrahan and Scholte.

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