1. Academic Validation
  2. Structure, synthesis, and molecular cloning of dermaseptins B, a family of skin peptide antibiotics

Structure, synthesis, and molecular cloning of dermaseptins B, a family of skin peptide antibiotics

  • J Biol Chem. 1998 Jun 12;273(24):14690-7. doi: 10.1074/jbc.273.24.14690.
S Charpentier 1 M Amiche J Mester V Vouille J P Le Caer P Nicolas A Delfour
Affiliations

Affiliation

  • 1 Laboratoire de Bioactivation des Peptides, Institut Jacques Monod, 2 Place Jussieu, 75251 Paris Cedex 05, France.
Abstract

Analysis of antimicrobial activities that are present in the skin secretions of the South American frog Phyllomedusa bicolor revealed six polycationic (lysine-rich) and amphipathic alpha-helical Peptides, 24-33 residues long, termed dermaseptins B1 to B6, respectively. Prepro-dermaseptins B all contain an almost identical signal peptide, which is followed by a conserved acidic propiece, a processing signal Lys-Arg, and a dermaseptin progenitor sequence. The 22-residue signal peptide plus the first 3 residues of the acidic propiece are encoded by conserved nucleotides encompassed by the first coding exon of the dermaseptin genes. The 25-residue amino-terminal region of prepro-dermaseptins B shares 50% identity with the corresponding region of precursors for D-amino acid containing opioid Peptides or for antimicrobial Peptides originating from the skin of distantly related frog species. The remarkable similarity found between prepro-proteins that encode end products with strikingly different sequences, conformations, biological activities and modes of action suggests that the corresponding genes have evolved through dissemination of a conserved "secretory cassette" exon.

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