Bifunctional glycolipids targeting TLR4·MD-2 and short pentraxins
Daniele Zucchetta, Lena Nuschy, Simon Gumpelmair, Peter Steinberger, Iain Wilson, Holger Heine, Alla Zamyatina

TL;DR
Researchers developed glycolipids that target immune receptors and proteins, reducing inflammation while interacting with immune system components.
Contribution
The study introduces PE-modified glycolipids that act as TLR4 antagonists and are recognized by human pentraxins.
Findings
PE-modified glycolipids reduce cytokine secretion in human mononuclear cells at micromolar levels.
Zwitterionic glycolipids are recognized and bound by human pentraxins CRP and SAP.
PE modification alters glycolipid aggregation and enables selective recognition by pentraxins.
Abstract
Innate immune detection of pathogen- and danger-associated molecular patterns (PAMPs/DAMPs) centres on pattern-recognition receptors, with the TLR4/MD-2 complex being uniquely sensitive to trace levels of lipopolysaccharide (LPS) as well as infection-triggered endogenous ligands. While this axis rapidly induces protective cytokine production and upregulation of co-stimulatory molecules, its malfunction can cause pathological hyperinflammation culminating in systemic inflammatory response syndrome (SIRS), highlighting the importance of the development of TLR4 antagonists for the management of immunopathological disorders. Cationic antimicrobial peptides (CAMPs) naturally neutralise LPS by engaging the anionic phosphate groups of lipid A; however, many bacteria evade CAMPs by masking these phosphates with phosphoethanolamine (PE), thereby attenuating electrostatic recognition. In…
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Taxonomy
TopicsImmune Response and Inflammation · Biomarkers in Disease Mechanisms · Macrophage Migration Inhibitory Factor
