Barbara La Ferla; Alice Paiotta; Giuseppe D'Orazio; Roberta Palorini; Francesca Ricciardiello; Luca Zoia; Giuseppina Votta; Luca De Gioia; Ferdinando Chiaradonna
Index: 10.1002/ejoc.201800183
Full Text: HTML
A library of GlcNAc‐6 or 1P analogues was designed and each compound was computationally evaluated through docking studies for its binding affinity to AGM1/PGM3. The compounds with the highest binding affinity ranked through a docking score, were synthesized and screened for their ability to inhibit the production of UDP‐GlcNAc. A glycofused oxazoline analogue showed a good inhibition ability and afforded significant results in vitro.
|
Development of Photoactivatable Nitroxyl (HNO) Donors Incorp...
2018-04-15 [10.1002/ejoc.201800092] |
|
Catalytic C‐Alkylation of Pyrroles with Primary Alcohols: Ha...
2018-03-30 [10.1002/ejoc.201800146] |
|
Fluorine‐Containing Functionalized Cyclopentene Scaffolds Th...
2018-03-30 [10.1002/ejoc.201800057] |
|
Verdazyl Radical Building Blocks: Synthesis, Structure, and ...
2018-03-30 [10.1002/ejoc.201701783] |
|
Iron‐Catalyzed Sulfur‐Promoted Decyanative Redox Condensatio...
2018-03-30 [10.1002/ejoc.201701607] |
Home | MSDS/SDS Database Search | Journals | Product Classification | Biologically Active Compounds | Selling Leads | About Us | Disclaimer
Copyright © 2024 ChemSrc All Rights Reserved