| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 5264847 | Tetrahedron Letters | 2013 | 4 Pages |
Abstract
C3-modified Neu5Ac2en derivatives can be used to study the flexible 150-loop region of influenza virus sialidases and also provide a new template for the development of next-generation sialidase inhibitors. This Letter describes an efficient synthetic route towards the large scale synthesis of C3 C-alkylated Neu5Ac2en derivatives. The key intermediate, a 3-eq-allyl-Neu5Ac derivative, is formed by stereoselective addition of the allyl group in an equatorial configuration at C3, regardless of the stereochemistry of the bromohydrin precursor.
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Authors
Santosh Rudrawar, Mauro Pascolutti, Beenu Bhatt, Robin J. Thomson, Mark von Itzstein,