Immunomodulation by lipid emulsions in pulmonary inflammation: a randomized controlled trial

Matthias Hecker; Tomke Linder; Juliane Ott; Hans-Dieter Walmrath; Jürgen Lohmeyer; István Vadász; Leigh M Marsh; Susanne Herold; Martin Reichert; Anja Buchbinder; Rory Edward Morty; Britta Bausch; Tobias Fischer; Richard Schulz; Friedrich Grimminger; Martin Witzenrath; Matt Barnes; Werner Seeger; Konstantin Mayer

doi:10.1186/s13054-015-0933-6

Immunomodulation by lipid emulsions in pulmonary inflammation: a randomized controlled trial

Crit Care. 2015 May 12;19(1):226. doi: 10.1186/s13054-015-0933-6.

Authors

Matthias Hecker¹, Tomke Linder², Juliane Ott³, Hans-Dieter Walmrath⁴, Jürgen Lohmeyer⁵, István Vadász⁶, Leigh M Marsh⁷, Susanne Herold⁸, Martin Reichert⁹, Anja Buchbinder¹⁰, Rory Edward Morty¹¹, Britta Bausch¹², Tobias Fischer¹³, Richard Schulz¹⁴, Friedrich Grimminger¹⁵, Martin Witzenrath¹⁶, Matt Barnes¹⁷, Werner Seeger¹⁸, Konstantin Mayer^{19

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Affiliations

¹ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. matthias.hecker@innere.med.uni-giessen.de.
² University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. tomke.linder@googlemail.com.
³ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. juliane.ott@innere.med.uni-giessen.de.
⁴ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. hans.dieter.walmrath@innere.med.uni-giessen.de.
⁵ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. juergen.lohmeyer@innere.med.uni-giessen.de.
⁶ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. istvan.vadasz@innere.med.uni-giessen.de.
⁷ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. leigh.marsh@lvr.lbg.ac.at.
⁸ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. susanne.herold@innere.med.uni-giessen.de.
⁹ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. martin86reichert@web.de.
¹⁰ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. anja.buchbinder@innere.med.uni-giessen.de.
¹¹ Department of Lung Development and Remodelling, Max Planck Institute for Heart and Lung Research, Bad Nauheim, Germany. rory.morty@innere.med.uni-giessen.de.
¹² University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. Britta.Bausch@web.de.
¹³ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. tobiasfischer.home@web.de.
¹⁴ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. richard.schulz@innere.med.uni-giessen.de.
¹⁵ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. friedrich.grimminger@innere.med.uni-giessen.de.
¹⁶ Charité - Universitätsmedizin Berlin, Medizinische Klinik mit Schwerpunkt Infektiologie und Pneumologie, Berlin, Germany. martin.witzenrath@charite.de.
¹⁷ Takeda Cambridge Ltd, Cambridge, UK. mbarnes@takedacam.com.
¹⁸ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. werner.seeger@innere.med.uni-giessen.de.
¹⁹ University of Giessen and Marburg Lung Center (UGMLC), Justus-Liebig-University of Giessen, Klinikstr. 33, Giessen, D - 35392, Germany. konstantin.mayer@innere.med.uni-giessen.de.
²⁰ University of Giessen and Marburg Lung Center (UGMLC), Medical Clinic II, Klinikstr. 33, Giessen, 35392, Germany. konstantin.mayer@innere.med.uni-giessen.de.

Abstract

Introduction: Acute respiratory distress syndrome (ARDS) is a major cause of mortality in intensive care units. As there is rising evidence about immuno-modulatory effects of lipid emulsions required for parenteral nutrition of ARDS patients, we sought to investigate whether infusion of conventional soybean oil (SO)-based or fish oil (FO)-based lipid emulsions rich in either n-6 or n-3 fatty acids, respectively, may influence subsequent pulmonary inflammation.

Methods: In a randomized controlled, single-blinded pilot study, forty-two volunteers received SO, FO, or normal saline for two days. Thereafter, volunteers inhaled pre-defined doses of lipopolysaccharide (LPS) followed by bronchoalveolar lavage (BAL) 8 or 24 h later. In the murine model of LPS-induced lung injury a possible involvement of resolvin E1 (RvE1) receptor ChemR23 was investigated. Wild-type and ChemR23 knockout mice were infused with both lipid emulsions and challenged with LPS intratracheally.

Results: In volunteers receiving lipid emulsions, the fatty acid profile in the plasma and in isolated neutrophils and monocytes was significantly changed. Adhesion of isolated monocytes to endothelial cells was enhanced after infusion of SO and reduced by FO, however, no difference of infusion on an array of surface adhesion molecules was detected. In neutrophils and monocytes, LPS-elicited generation of pro-inflammatory cytokines increased in the SO and decreased in the FO group. LPS inhalation in volunteers evoked an increase in neutrophils in BAL fluids, which decreased faster in the FO group. While TNF-α in the BAL was increased in the SO group, IL-8 decreased faster in the FO group. In the murine model of lung injury, effects of FO similar to the volunteer group observed in wild-type mice were abrogated in ChemR23 knockout mice.

Conclusions: After infusion of conventional lipid emulsions, leukocytes exhibited increased adhesive and pro-inflammatory features. In contrast, FO-based lipid emulsions reduced monocyte adhesion, decreased pro-inflammatory cytokines, and neutrophil recruitment into the alveolar space possibly mediated by ChemR23-signaling. Lipid emulsions thus exert differential effects in human volunteers and mice in vivo.

Trial registration: DRKS00006131 at the German Clinical Trial Registry, 2014/05/14.

Publication types

Randomized Controlled Trial
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Cells, Cultured
Fat Emulsions, Intravenous / administration & dosage*
Fish Oils / administration & dosage
Humans
Immunomodulation / drug effects*
Immunomodulation / immunology*
Inflammation Mediators / antagonists & inhibitors
Inflammation Mediators / immunology
Mice
Mice, Knockout
Pilot Projects
Pneumonia / drug therapy*
Pneumonia / immunology*
Single-Blind Method
Soybean Oil / administration & dosage

Substances

Fat Emulsions, Intravenous
Fish Oils
Inflammation Mediators
Soybean Oil

Associated data

DRKS/DRKS00006131