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Curr Protein Pept Sci


Title:Peptide AS-48: prototype of a new class of cyclic bacteriocins
Author(s):Maqueda M; Galvez A; Bueno MM; Sanchez-Barrena MJ; Gonzalez C; Albert A; Rico M; Valdivia E;
Address:"Dpto. Microbiologia, Facultad de Ciencias, Universidad de Granada, 18071 Granada, Spain. mmaqueda @ugr.es"
Journal Title:Curr Protein Pept Sci
Year:2004
Volume:5
Issue:5
Page Number:399 - 416
DOI: 10.2174/1389203043379567
ISSN/ISBN:1389-2037 (Print) 1389-2037 (Linking)
Abstract:"After the discovery of bacteriocin AS-48, a 70-residue cyclic peptide produced by Enterococcus faecalis subsp. liquefaciens, some naturally-occurring cyclic proteins from bacteria have been reported. AS-48 is encoded by the 68-kb pheromone-responsive plasmid pMB2, and the gene cluster involved in production and immunity has been identified and sequenced. This peptide exerts a bactericidal action on sensitive cells (most of the Gram-positive and some Gram-negative bacteria). Its target is the cytoplasmic membrane, in which it opens pores, leading to the dissipation of the proton motive force and cell death, a mechanism similar to that proposed for the action of defensins or, most generally, cationic antibacterial peptides. This fact, together with its remarkable stability and solubility over a wide pH range, suggest that this bacteriocin could be a good candidate as a natural food preservative. The amino acid composition of purified AS-48 shows the absence of modified or dehydrated residues, making it clearly different from lantibiotics. Bacteriocin AS-48 also differs from defensins in that it does not contain cysteines and consequently no disulfide bridges, which makes is high stability even more remarkable. Composition analysis of AS-48 shows a high proportion of basic to acidic amino acids, conferring to this peptide a strong basic character, with an isoelectric point close to 10.5. Determination of the AS-48 structural gene DNA sequence, together with the sequences of AS-48 protease digestion fragments and mass spectrometry determinations, allowed us to determine unambiguously the cyclic structure of the molecule, being the first example of a posttranslational modification in which a cyclic structure arises from a 'head-to-tail' linkage. We have solved the three-dimensional structure of AS-48 in solution, and it consists of a globular arrangement of five alpha-helices enclosing a compact hydrophobic core. Interestingly, the head-to-tail peptide link between Trp-70 and Met-1 lies in the middle of alpha-helix 5, which is shown to have a pronounced effect on the stability of the three-dimensional structure. Analysis of structure-function relationship allowed us to propose models to understand the aspects of the molecular function of AS-48. The purpose of this work is to review recent developments in our understanding about the biochemical and biological characteristics and structure of this unusual type of bacteriocin"
Keywords:"Animals Anti-Bacterial Agents/*chemistry/immunology/isolation & purification/*pharmacology Bacteriocins/*chemistry/immunology/isolation & purification/*pharmacology Models, Molecular Peptides, Cyclic/*chemistry/immunology/*pharmacology Protein Structure, ;"
Notes:"MedlineMaqueda, Mercedes Galvez, Antonio Bueno, Manuel Martinez Sanchez-Barrena, Maria Jose Gonzalez, Carlos Albert, Armando Rico, Manuel Valdivia, Eva eng Research Support, Non-U.S. Gov't Review United Arab Emirates 2004/11/17 Curr Protein Pept Sci. 2004 Oct; 5(5):399-416. doi: 10.2174/1389203043379567"

 
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Citation: El-Sayed AM 2024. The Pherobase: Database of Pheromones and Semiochemicals. <http://www.pherobase.com>.
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