Literature DB >> 25394365

Anti-endotoxic activity and structural basis for human MD-2·TLR4 antagonism of tetraacylated lipid A mimetics based on βGlcN(1↔1)αGlcN scaffold.

Jose Antonio Garate1, Johannes Stöckl2, María del Carmen Fernández-Alonso3, Daniel Artner4, Mira Haegman5, Chris Oostenbrink1, Jesús Jiménez-Barbero3, Rudi Beyaert5, Holger Heine6, Paul Kosma4, Alla Zamyatina7.   

Abstract

Interfering with LPS binding by the co-receptor protein myeloid differentiation factor 2 (MD-2) represents a useful approach for down-regulation of MD-2·TLR4-mediated innate immune signaling, which is implicated in the pathogenesis of a variety of human diseases, including sepsis syndrome. The antagonistic activity of a series of novel synthetic tetraacylated bis-phosphorylated glycolipids based on the βGlcN(1↔1)αGlcN scaffold was assessed in human monocytic macrophage-like cell line THP-1, dendritic cells and human epithelial cells. Two compounds were shown to inhibit efficiently the LPS-induced inflammatory signaling by down-regulation of the expression of TNF-α, IL-6, IL-8, IL-10 and IL-12 to background levels. The binding of the tetraacylated by (R)-3-hydroxy-fatty acids (2 × C12, 2 × C14), 4,4'-bisphosphorylated βGlcN(1↔1)αGlcN-based lipid A mimetic DA193 to human MD-2 was calculated to be 20-fold stronger than that of Escherichia coli lipid A. Potent antagonistic activity was related to a specific molecular shape induced by the β,α(1↔1)-diglucosamine backbone. 'Co-planar' relative arrangement of the GlcN rings was inflicted by the double exo-anomeric conformation around both glycosidic torsions in the rigid β,α(1↔1) linkage, which was ascertained using NOESY NMR experiments and confirmed by molecular dynamics simulation. In contrast to the native lipid A ligands, the binding affinity of βGlcN(1↔1)αGlcN-based lipid A mimetics to human MD-2 was independent on the orientation of the diglucosamine backbone of the synthetic antagonist within the binding pocket of hMD-2 (rotation by 180°) allowing for two equally efficient binding modes as shown by molecular dynamics simulation.
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Entities:  

Keywords:  Antagonist; MD-2; NMR; Toll-like receptor 4; glycolipids; lipid A; lipopolysaccharide; molecular dynamics simulation

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Year:  2014        PMID: 25394365      PMCID: PMC4452626          DOI: 10.1177/1753425914550426

Source DB:  PubMed          Journal:  Innate Immun        ISSN: 1753-4259            Impact factor:   2.680


  39 in total

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6.  Endotoxin: physical requirements for cell activation.

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Journal:  J Biol Chem       Date:  2009-03-24       Impact factor: 5.157

9.  Influence of the supramolecular structure of free lipid A on its biological activity.

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Authors:  Kari Ann Shirey; Wendy Lai; Alison J Scott; Michael Lipsky; Pragnesh Mistry; Lioubov M Pletneva; Christopher L Karp; Jaclyn McAlees; Theresa L Gioannini; Jerrold Weiss; Wilbur H Chen; Robert K Ernst; Daniel P Rossignol; Fabian Gusovsky; Jorge C G Blanco; Stefanie N Vogel
Journal:  Nature       Date:  2013-05-01       Impact factor: 49.962

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  6 in total

1.  Lipid A Mimetics Based on Unnatural Disaccharide Scaffold as Potent TLR4 Agonists for Prospective Immunotherapeutics and Adjuvants.

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2.  Synthetic glycan-based TLR4 agonists targeting caspase-4/11 for the development of adjuvants and immunotherapeutics.

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Review 3.  Lipopolysaccharide Recognition in the Crossroads of TLR4 and Caspase-4/11 Mediated Inflammatory Pathways.

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4.  Exploring electrostatic patterns of human, murine, equine and canine TLR4/MD-2 receptors.

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Journal:  Innate Immun       Date:  2019-12-25       Impact factor: 2.680

5.  Tailored Modulation of Cellular Pro-inflammatory Responses With Disaccharide Lipid A Mimetics.

Authors:  Holger Heine; Florian Adanitsch; Tina Tinkara Peternelj; Mira Haegman; Christoph Kasper; Simon Ittig; Rudi Beyaert; Roman Jerala; Alla Zamyatina
Journal:  Front Immunol       Date:  2021-03-18       Impact factor: 7.561

6.  Shortening the Lipid A Acyl Chains of Bordetella pertussis Enables Depletion of Lipopolysaccharide Endotoxic Activity.

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Journal:  Vaccines (Basel)       Date:  2020-10-09
  6 in total

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