Structure-Activity Relationship in Monosaccharide-Based Toll-Like Receptor 4 (TLR4) Antagonists.
Fabio Alessandro FacchiniLenny ZaffaroniAlberto MinottiSilvia RapisardaValentina CalabreseMatilde ForcellaPaola FusiCristina AiroldiCarlotta CiaramelliJean-Marc BillodAndra B SchrommHarald BraunCharys PalmerRudi BeyaertFabio LapentaRoman JeralaGrisha PirianovSonsoles Martin-SantamariaFrancesco PeriPublished in: Journal of medicinal chemistry (2018)
The structure-activity relationship was investigated in a series of synthetic TLR4 antagonists formed by a glucosamine core linked to two phosphate esters and two linear carbon chains. Molecular modeling showed that the compounds with 10, 12, and 14 carbons chains are associated with higher stabilization of the MD-2/TLR4 antagonist conformation than in the case of the C16 variant. Binding experiments with human MD-2 showed that the C12 and C14 variants have higher affinity than C10, while the C16 variant did not interact with the protein. The molecules, with the exception of the C16 variant, inhibited the LPS-stimulated TLR4 signal in human and murine cells, and the antagonist potency mirrored the MD-2 affinity calculated from in vitro binding experiments. Fourier-transform infrared, nuclear magnetic resonance, and small angle X-ray scattering measurements suggested that the aggregation state in aqueous solution depends on fatty acid chain lengths and that this property can influence TLR4 activity in this series of compounds.
Keyphrases
- toll like receptor
- inflammatory response
- structure activity relationship
- nuclear factor
- immune response
- magnetic resonance
- endothelial cells
- fatty acid
- aqueous solution
- high resolution
- molecular dynamics
- induced apoptosis
- pluripotent stem cells
- computed tomography
- cell cycle arrest
- contrast enhanced
- signaling pathway
- transcription factor
- oxidative stress
- small molecule
- anti inflammatory
- high speed
- dual energy
- protein protein