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Mixed Oligoureas Based on Constrained Bicyclic and Acyclic β‐Amino Acids Derivatives: On the Significance of the Subunit Configuration for Folding
Authors:Dr Christophe André  Dr Baptiste Legrand  Laure Moulat  Emmanuel Wenger  Dr Claude Didierjean  Dr Emmanuel Aubert  Dr Marie Christine Averlant‐Petit  Prof Jean Martinez  Dr Muriel Amblard  Dr Monique Calmes
Institution:1. IBMM, UMR 5247 CNRS, Universités Montpellier 1 et 2, 15 avenue Charles Flahault, 34093 Montpellier Cedex 5 (France);2. CRM2, UMR 7063 CNRS Université de Lorraine, Boulevard des Aiguilletes, 54506 Vandoeuvre‐lès‐Nancy Cedex (France);3. LCPM ‐ UMR 7568 CNRS Université de Lorraine, 1 rue Grandville, 54001 Nancy Cedex 1 (France)
Abstract:The combination of a non‐functionalized constrained bicyclo2.2.2]octane motif along with urea linkages allowed the formation of a highly rigid 2.512/14 helical system both in solution and the solid state. In this work, we aimed at developing stable and functionalized systems as promising materials for biological applications in investigating the impact of this constrained motif and its configuration on homo and heterochiral mixed‐oligourea helix formation. Di‐, tetra‐, hexa‐, and octa‐oligoureas alternating the highly constrained bicyclic motif of (R) or (S) configuration with acyclic (S)‐β3‐amino acid derivatives were constructed. Circular dichroism (CD), NMR experiments, and the X‐ray crystal structure of the octamer unequivocally proved that the alternating heterochiral R/S sequences form a stable left‐handed 2.5‐helix in contrast to the mixed (S/S)‐oligoureas, which did not adopt any defined secondary structure. We observed that the (?)‐synclinal conformation around the Cα? Cβ bond of the acyclic residues, although sterically less favorable than the (+)‐synclinal conformation, was imposed by the (R)‐bicyclic amino carbamoyl (BAC) residue. This highlighted the strong ability of the BAC residue to drive helical folding in heterochiral compounds. The role of the stereochemistry of the BAC unit was assessed and a model was proposed to explain the misfolding of the S/S sequences.
Keywords:bicyclic β  ‐amino acid derivatives  conformation analysis  foldamers  mixed oligoureas  helical structures
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