Cathelicidin and PMB neutralize endotoxins by multifactorial mechanisms including LPS interaction and targeting of host cell membranes

Author:

Schromm Andra B.ORCID,Paulowski Laura,Kaconis Yani,Kopp Franziska,Koistinen Max,Donoghue Annemarie,Keese Susanne,Nehls ChristianORCID,Wernecke Julia,Garidel PatrickORCID,Sevcsik EvaORCID,Lohner Karl,Sanchez-Gomez SusanaORCID,Martinez-de-Tejada GuillermoORCID,Brandenburg Klaus,Brameshuber MarioORCID,Schütz Gerhard J.ORCID,Andrä Jörg,Gutsmann Thomas

Abstract

Antimicrobial peptides (AMPs) contribute to an effective protection against infections. The antibacterial function of AMPs depends on their interactions with microbial membranes and lipids, such as lipopolysaccharide (LPS; endotoxin). Hyperinflammation induced by endotoxin is a key factor in bacterial sepsis and many other human diseases. Here, we provide a comprehensive profile of peptide-mediated LPS neutralization by systematic analysis of the effects of a set of AMPs and the peptide antibiotic polymyxin B (PMB) on the physicochemistry of endotoxin, macrophage activation, and lethality in mice. Mechanistic studies revealed that the host defense peptide LL-32 and PMB each reduce LPS-mediated activation also via a direct interaction of the peptides with the host cell. As a biophysical basis, we demonstrate modifications of the structure of cholesterol-rich membrane domains and the association of glycosylphosphatidylinositol (GPI)-anchored proteins. Our discovery of a host cell–directed mechanism of immune control contributes an important aspect in the development and therapeutic use of AMPs.

Funder

Deutsche Forschungsgemeinschaft

Universidad de Navarra

Ministerio de Sanidad y Consumo, Spain

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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