doi: 10.1016/j.bmc.2011.08.032.
Epub 2011 Aug 22.
Design and synthesis of inhibitors of noroviruses by scaffold hopping
Affiliations
- PMID: 21893416
- PMCID: PMC3199213
- DOI: 10.1016/j.bmc.2011.08.032
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Design and synthesis of inhibitors of noroviruses by scaffold hopping
Bioorg Med Chem.
.
Abstract
A scaffold hopping strategy was employed to identify new chemotypes that inhibit noroviruses. The replacement of the cyclosulfamide scaffold by an array of heterocyclic scaffolds lead to the identification of additional series of compounds that possessed anti-norovirus activity in a cell-based replicon system.
Copyright © 2011 Elsevier Ltd. All rights reserved.
Figures
Norovirus inhibitor scaffold hopping strategy.
Reaction conditions: i) CDI/1,4-dioxane; ii) BrCH2COOC(CH3)3/DMF/0°C to rt; iii) TFA; iv) SOCl2/CH3OH; v) LiBH4/THF/EtOH; vi) MsCl/TEA/CH2Cl2; vii) 1eq morpholine or 0.5 eq piperazine, NaHCO3/95% EtOH/reflux.
Reaction conditions: i) NaBH4/MeOH; ii) NH2SO4NH2/pyridine/reflux 16h; iii) CDI/1,4-dioxance
Reaction conditions: i) NBS/AIBN/CCl4; ii) NaN3/DMSO; iii) R1C≡ CH/Sodium ascorbate/CuSO4/t-BuOH:H2O(1:1) or CuI/DMSO; iv) TBAF/THF; v) NaCN/DMSO; vi) NaN3/NH4Cl/DMF/100 °C; vii) CH3I/TEA/ACN; viii) CDI/THF/ACN.
Reaction conditions: i) Gly-OCH3(HCl)/TEA/NaBH4/CH3OH; ii) a) ClSO2NCO/t-BuOH/CH2Cl2, b) TEA/CH2Cl2; iii) TFA; iv) NaH/THF.
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