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Binding between lipopolysaccharide and cecropin A
Authors:Anthony J. De Lucca  Thomas J. Jacks  Kim A. Brogden
Affiliation:(1) Southern Regional Research Center, USDA, ARS, 1100 Robert E. Lee Boulevards, 70124-4305 New Orleans, LA, USA;(2) National Animal Disease Center, USDA, ARS, 2300 Dayton Avenue, 50010 Ames, IA, USA
Abstract:Cecropin A (CA), a bioactive peptide, produced significant lethality toPantoea agglomerans (PA) at low concentrations. Significant mortality occurred immediately after addition of CA. Separate preincubations of lipopolysaccharides (LPS) from the following bacteria: PA,Serratia marcescens, Escherichia coli (EC), andSalmonella typhimurium with CA were performed prior to the bioassay. CA was also preincubated with diphosphoryl lipid A (DPL-A) from EC andS. minnesota (SM), trilinolein, palmitic, lauric and myristic acids (fatty acids contained in the lipid A of PA-LPS) and bovine brain gangliosides. Spectral analyses to determine the interaction between glycosphingolipids (sphingomyelin, bovine brain gangliosides, and galactocerebrosides) and CA were performed. Results showed that all types of LPS and DPL-A as well as the gangliosides studied blocked CA lethality to PA. The level of inhibition of CA antibacterial properties was dependent on LPS and DPL-A concentration. The individual fatty acids and trilinolein did not affect CA lethality to PA. Spectral studies showed complexation between CA and PA-LPS, both types of DPL-A, and the glycosphingolipids. Biological and chemical analyses confirm that CA binds to the diphosphoryl lipid A moiety of LPS.The U.S. Government right to retain a non-exclusive, royalty free licence in and to any copyright is acknowledged
Keywords:cecropin A  peptide  lipopolysaccharide  lipid A  binding
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