Alveolar type II epithelial cell FASN maintains lipid homeostasis in experimental COPD
Li-Chao Fan, … , Jin-Fu Xu, Suzanne M. Cloonan
Li-Chao Fan, … , Jin-Fu Xu, Suzanne M. Cloonan
Published August 22, 2023
Citation Information: JCI Insight. 2023;8(16):e163403. https://doi.org/10.1172/jci.insight.163403.
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Research Article Metabolism Pulmonology

Alveolar type II epithelial cell FASN maintains lipid homeostasis in experimental COPD

Abstract

Alveolar epithelial type II (AEC2) cells strictly regulate lipid metabolism to maintain surfactant synthesis. Loss of AEC2 cell function and surfactant production are implicated in the pathogenesis of the smoking-related lung disease chronic obstructive pulmonary disease (COPD). Whether smoking alters lipid synthesis in AEC2 cells and whether altering lipid metabolism in AEC2 cells contributes to COPD development are unclear. In this study, high-throughput lipidomic analysis revealed increased lipid biosynthesis in AEC2 cells isolated from mice chronically exposed to cigarette smoke (CS). Mice with a targeted deletion of the de novo lipogenesis enzyme, fatty acid synthase (FASN), in AEC2 cells (FasniΔAEC2) exposed to CS exhibited higher bronchoalveolar lavage fluid (BALF) neutrophils, higher BALF protein, and more severe airspace enlargement. FasniΔAEC2 mice exposed to CS had lower levels of key surfactant phospholipids but higher levels of BALF ether phospholipids, sphingomyelins, and polyunsaturated fatty acid–containing phospholipids, as well as increased BALF surface tension. FasniΔAEC2 mice exposed to CS also had higher levels of protective ferroptosis markers in the lung. These data suggest that AEC2 cell FASN modulates the response of the lung to smoke by regulating the composition of the surfactant phospholipidome.

Authors

Li-Chao Fan, Keith McConn, Maria Plataki, Sarah Kenny, Niamh C. Williams, Kihwan Kim, Jennifer A. Quirke, Yan Chen, Maor Sauler, Matthias E. Möbius, Kuei-Pin Chung, Estela Area Gomez, Augustine M.K. Choi, Jin-Fu Xu, Suzanne M. Cloonan

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Figure 7

Targeted deletion of FASN in AEC2 cells increases abundance of PUFA-bound lipids and increases markers of ferroptosis in response to smoke.

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Targeted deletion of FASN in AEC2 cells increases abundance of PUFA-boun...
(A) Volcano plot of significantly altered PUFA-containing phospholipids in the FasniΔAEC2 mice compared with SftpcCreERT2+/– control mice in response to 6 weeks of smoke (n = 4 per group). (B) Percentage abundance of saturated fatty acid–containing (SFA-containing), MUFA-containing, and PUFA-containing phosphatidylcholine species (calculated by expressing the concentration of each SFA, MUFA, and PUFA as a percentage of total phosphatidylcholine species). (C) Representative immunoblots (left) and relative quantification (right) for the ferroptosis markers, SLC7A11 and GPX4, with corresponding β-actin loading controls in FasniΔAEC2 mice compared with SftpcCreERT2+/– control mice in response to 6 months of smoke. Immunoblot representative of n = 2 mice per group; densitometry representative of n = 3–5 mice per group. Data represented as mean ± SEM of 1 independent experiment. *P < 0.05 by 1-way ANOVA followed by Tukey’s correction.