Titz, Bjoern; Boué, Stéphanie; Phillips, Blaine; Talikka, Marja; Vihervaara, Terhi; Schneider, Thomas; Nury, Catherine; Elamin, Ashraf; Guedj, Emmanuel; Peck, Michael J.; Schlage, Walter K.; Cabanski, Maciej; Leroy, Patrice; Vuillaume, Gregory; Martin, Florian; Martin, Nikolai V.; Veljkovic, Emilija; Kim Ekroos; Laaksonen, Reijo; Vanscheeuwijck, Patrick

doi:10.1093/toxsci/kfv244

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Title: Effects of Cigarette Smoke, Cessation, and Switching to Two Heat-Not-Burn Tobacco Products on Lung Lipid Metabolism in C57BL/6 and Apoe<sup>-/-</sup> Mice-An Integrative Systems Toxicology Analysis.
Authors: Titz, Bjoern; Boué, Stéphanie; Phillips, Blaine; Talikka, Marja; Vihervaara, Terhi; Schneider, Thomas; Nury, Catherine; Elamin, Ashraf; Guedj, Emmanuel; Peck, Michael J.; Schlage, Walter K.; Cabanski, Maciej; Leroy, Patrice; Vuillaume, Gregory; Martin, Florian; Martin, Nikolai V.; Veljkovic, Emilija; Kim Ekroos; Laaksonen, Reijo; Vanscheeuwijck, Patrick
Abstract: The impact of cigarette smoke (CS), a major cause of lung diseases, on the composition and metabolism of lung lipids is incompletely understood. Here, we integrated quantitative lipidomics and proteomics to investigate exposure effects on lung lipid metabolismin a C57BL/6 and an Apolipoprotein E-deficient (Apoe-/-) mouse study. In these studies, mice were exposed to high concentrations of 3R4F reference CS, aerosol from potential modified risk tobacco products (MRTPs) or filtered air (Sham) for up to 8 months. The 2 assessed MRTPs, the prototypical MRTP for C57BL/6 mice and the Tobacco Heating System 2.2 for Apoe-/- mice, utilize"heat-not-burn" technologies and were each matched in nicotine concentrations to the 3R4F CS. After 2 months of CS exposure, some groups were either switched to the MRTP or underwent cessation. In both mouse strains, CS strongly affected several categories of lung lipids and lipid-related proteins. Candidate surfactant lipids, surfactant proteins, and surfactant metabolizing proteins were increased. Inflammatory eicosanoids, their metabolic enzymes, and several ceramide classes were elevated. Overall, CS induced a coordinated lipid response controlled by transcription regulators such as SREBP proteins and supported by other metabolic adaptations. In contrast, most of these changes were absent in the mice exposed to the potential MRTPs, in the cessation group, and the switching group. Our findings demonstrate the complex biological response of the lungs to CS exposure and support the benefits of cessation or switching to a heat-not-burn product using a design such as those employed in this study.
Subjects: CIGARETTE smokers -- Risk factors; CIGARETTE smokers; TOBACCO products; TOXICOLOGY; LIPID metabolism
Publication: Toxicological Sciences, 2016, Vol 149, Issue 2, p441
ISSN: 1096-6080
Publication type: Academic Journal
DOI: 10.1093/toxsci/kfv244

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Effects of Cigarette Smoke, Cessation, and Switching to Two Heat-Not-Burn Tobacco Products on Lung Lipid Metabolism in C57BL/6 and Apoe<sup>-/-</sup> Mice-An Integrative Systems Toxicology Analysis.

CIGARETTE smokers -- Risk factors; CIGARETTE smokers; TOBACCO products; TOXICOLOGY; LIPID metabolism

Toxicological Sciences, 2016, Vol 149, Issue 2, p441

1096-6080

Academic Journal

10.1093/toxsci/kfv244