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Biophysical Journal 63: 868-873 (1992)
© 1992 the Biophysical Society

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Prolines are not essential residues in the "barrel-stave" model for ion channels induced by alamethicin analogues.

H Duclohier, G Molle, J Y Dugast and G Spach

URA 500 CNRS, Faculté des Sciences, Université de Rouen, Mont-Saint-Aignan, France.

ABSTRACT

In the "barrel-stave" model for voltage-gated alamethicin channels in planar lipid bilayers, proline residues, especially Pro14, are assumed to play a significant role. Taking advantage of a previous synthetic alamethicin analogue in which all eight alpha-aminoisobutyric acids were replaced by leucines, two new analogues were prepared in order to test the effects of Pro14 and Pro2 substitutions by alanines. The alpha-helical content of the three analogues in methanol solution remains predominant (between 63 and 80%). Macroscopic conductance experiments show that a high voltage dependence is conserved, although the apparent mean number of monomers forming the channels is significantly reduced when the substitution occurs at position 14. This is confirmed in single-channel experiments which further reveal faster fluctuations for the modified analogues. These results demonstrate that, although prolines, especially Pro14, are favorable residues for alamethicin-like events, they are not absolute prerequisites for the development of highly voltage-dependent multistate conductances.







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Copyright © 1992 by the Biophysical Society.