TY - JOUR
T1 - “Double-click” protocol for synthesis of heterobifunctional multivalent ligands: Toward a focused library of specific norovirus inhibitors
AU - Guiard, Julie
AU - Fiege, Brigitte
AU - Kitov, Pavel I.
AU - Peters, Thomas
AU - Bundle, David R.
N1 - Funding Information:
Financial support for J.G., P.I.K., and D.R.B. was provided by the Alberta Innovates Centre for Carbohydrate Science and the Natural Science and Engineering Research Council of Canada. T.P. thanks the Deutsche Forschungsgemeinschaft (DFG) for grant Pe494/8-1 and for grants HBFG 101/192-1 and ME 1830/1. B.F. thanks the Studienstiftung des deutschen Volkes for a stipend.
Copyright:
Copyright 2017 Elsevier B.V., All rights reserved.
PY - 2011/6/27
Y1 - 2011/6/27
N2 - Researchers synrhesized hetero-bifunctional ligands either presented on a polymeric scaffold or as univalent monomers for STD NMR studies. All derivatives contained an invariant moiety, the α-L-fucose, and differ in the second variable ligand, a non-carbohydrate molecule selected by STD NMR screening of the Maybridge compound library. The detailed account of this screening, which directed he design of the hetero-bifunctional ligands, together with NMR studies of the univalent monomers is reported in the accompanying manuscript. The first compund was was obtained by Fisher glycosidation of lfucose with propargyl alcohol, by using sulfuric acid immobilized on silica as a catalyst. This method provided the desired glycoside in a 4:1 (α/Β) ratio. After peracetylation, the α anomer was easily purified from an (α/Β) mixture of triacetates. Trans-esterification afforded compound 2 in 50% overall yield.
AB - Researchers synrhesized hetero-bifunctional ligands either presented on a polymeric scaffold or as univalent monomers for STD NMR studies. All derivatives contained an invariant moiety, the α-L-fucose, and differ in the second variable ligand, a non-carbohydrate molecule selected by STD NMR screening of the Maybridge compound library. The detailed account of this screening, which directed he design of the hetero-bifunctional ligands, together with NMR studies of the univalent monomers is reported in the accompanying manuscript. The first compund was was obtained by Fisher glycosidation of lfucose with propargyl alcohol, by using sulfuric acid immobilized on silica as a catalyst. This method provided the desired glycoside in a 4:1 (α/Β) ratio. After peracetylation, the α anomer was easily purified from an (α/Β) mixture of triacetates. Trans-esterification afforded compound 2 in 50% overall yield.
UR - http://www.scopus.com/inward/record.url?scp=80054025249&partnerID=8YFLogxK
U2 - 10.1002/chem.201003414
DO - 10.1002/chem.201003414
M3 - Journal articles
C2 - 21469230
AN - SCOPUS:80054025249
SN - 0947-6539
VL - 17
SP - 7438
EP - 7441
JO - Chemistry - A European Journal
JF - Chemistry - A European Journal
IS - 27
ER -