| Literature DB >> 28004420 |
Flaviana Di Lorenzo1, Angelo Palmigiano2, Sami Al Bitar-Nehme3, Luisa Sturiale2, Katarzyna A Duda4, Djamel Gully5, Rosa Lanzetta1, Eric Giraud5, Domenico Garozzo2, Maria Lina Bernardini3,6, Antonio Molinaro1, Alba Silipo1.
Abstract
The search for novel lipid A analogues from any biological source that can act as antagonists, displaying inhibitory activity towards the production of pro-inflammatory cytokines, or as immunomodulators in mammals, is a very topical issue. To this aim, the structure and immunological properties of the lipopolysaccharide lipid A from the purple nonsulfur bacterium Rhodopseudomonas palustris strain BisA53 have been determined. This lipid A displays a unique structural feature, with a non-phosphorylated skeleton made up of the tetrasaccharide Manp-α-(1→4)-GlcpN3N-β-1→6-GlcpN3N-α-(1→1)-α-GalpA, and four primary amide-linked 14:0(3-OH) and, as secondary O-acyl substituents, a 16:0 and the very long-chain fatty acid 26:0(25-OAc), appended on the GlcpN3N units. This lipid A architecture is definitely rare, so far identified only in the genus Bradyrhizobium. Immunological tests on both murine bone-marrow-derived and human monocyte-derived macrophages revealed an extremely low immunostimulant capability of this LPS lipid A.Entities:
Keywords: NMR spectroscopy; fatty acids; glycolipids; innate immunity; lipopolysaccharides
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Year: 2016 PMID: 28004420 DOI: 10.1002/chem.201604379
Source DB: PubMed Journal: Chemistry ISSN: 0947-6539 Impact factor: 5.236