Trichogin GA IV, an 11-residue lipopeptaibol blocked at the N-terminus by an n-octanoyl group and at the C-terminus by a 1,2-amino alcohol (L-leucinol), extracted from the fungus Trichoderma longibrachiatum, exhibits remarkable membrane-modifying properties. We have synthesized trichogin GA IV and several [L-Leu-OMe(11)] analogs carrying at the N-terminus an acyl chain of variable length (C-2-C-8, C-10, C-12, C-14, C-16, C-18) A succinoylated head-to-head dimer was also prepared. A conformational analysis, carried out by FTIR absorption, CD, and NMR, showed that the right-handed helical structure of the natural lipopeptaibol is essentially preserved in all its analogs. Permeability measurements revealed that at least six carbon atoms in the N-alpha-blocking fatty acyl moiety are required for the onset of significant membrane-modifying properties. Also the head-to-head dimer is remarkably active. Possible models for the mechanism of membrane permeability of trichogin GA IV are discussed.

Effect of N-alpha-acyl chain length on the membrane-modifying properties of synthetic analogs of the lipopeptaibol trichogin GA IV

M Crisma;
1996

Abstract

Trichogin GA IV, an 11-residue lipopeptaibol blocked at the N-terminus by an n-octanoyl group and at the C-terminus by a 1,2-amino alcohol (L-leucinol), extracted from the fungus Trichoderma longibrachiatum, exhibits remarkable membrane-modifying properties. We have synthesized trichogin GA IV and several [L-Leu-OMe(11)] analogs carrying at the N-terminus an acyl chain of variable length (C-2-C-8, C-10, C-12, C-14, C-16, C-18) A succinoylated head-to-head dimer was also prepared. A conformational analysis, carried out by FTIR absorption, CD, and NMR, showed that the right-handed helical structure of the natural lipopeptaibol is essentially preserved in all its analogs. Permeability measurements revealed that at least six carbon atoms in the N-alpha-blocking fatty acyl moiety are required for the onset of significant membrane-modifying properties. Also the head-to-head dimer is remarkably active. Possible models for the mechanism of membrane permeability of trichogin GA IV are discussed.
1996
Inglese
118
4952
4958
Sì, ma tipo non specificato
Citazioni WOS: 54 Impact Factor 1996: 5.948 Coautore
1
info:eu-repo/semantics/article
262
C. Toniolo; M. Crisma; F. Formaggio; C. Peggion; V. Monaco; C. Goulard; S. Rebuffat; B. Bodo
01 Contributo su Rivista::01.01 Articolo in rivista
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/20.500.14243/175351
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