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1,3,5-Triazepane-2,6-diones as structurally diverse and conformationally constrained dipeptide mimetics: identification of malaria liver stage inhibitors from a small pilot library
Authors:Lena Gersande  Lallemand Eliette  Gruner Anne Charlotte  Boeglin Joel  Roussel Solveig  Schaffner Arnaud-Pierre  Aubry André  Franetich Jean-François  Mazier Dominique  Landau Irène  Briand Jean-Paul  Didierjean Claude  Rénia Laurent  Guichard Gilles
Affiliation:Immunologie et Chimie Thérapeutiques (ICT), UPR CNRS 9021, Institut de Biologie Moléculaire et Cellulaire, 15 rue Descartes, 67084 Strasbourg, France.
Abstract:The development of the 1,3,5-triazepane-2,6-dione system as a novel, conformationally restricted, and readily accessible class of dipeptidomimetics is reported. The synthesis of the densely functionalized 1,3,5-triazepane-2,6-dione skeleton was achieved in only four steps from a variety of simple linear dipeptide precursors. To extend the practical value of 1,3,5-triazepane-2,6-diones, a general polymer-assisted solution-phase synthesis approach amenable to library production in a multiparallel format was developed. The conformational preferences of the 1,3,5-triazepane-2,6-dione skeleton were investigated in detail by NMR spectroscopy and X-ray diffraction. The ring exhibits a characteristic folded conformation which was compared to that of related dipeptide-derived scaffolds including the more planar 2,5-diketopiperazine (DKP). Molecular and structural diversity was increased further through post-cyclization appending operations at urea nitrogens. Preliminary biological screens of a small collection of 1,3,5-triazepane-2,6-diones revealed inhibitors of the underexplored malaria liver stage and suggest strong potential for this dipeptide-derived scaffold to interfere with and to modulate biological pathways.
Keywords:heterocycles  molecular diversity  peptides  peptidomimetics  solid‐phase synthesis
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