摘要
An effective synthetic method for polyhydroxylated azepanes that contain an alkyl group (Me or Bu) at either the 7- or N-positions is developed. The synthetic routes are accomplished in eight to ten steps from d-(-)-quinic acid. Among the compounds synthesized, the polyhydroxy 7-butyl azepane (compound 3), which possessed the R-configuration at C-7 position, is shown to give potent inhibition against β-galactosidase (IC50 = 3 μM). Preliminary biological data indicate that the length of alkyl groups along with the proper stereochemistry at the C-7 position is essential for acquiring extra binding affinity. Using similar synthetic routes, the polyhydroxy N-methyl and N-butyl azepanes are synthesized for the comparison of their biological activities.
| 原文 | 英語 |
|---|---|
| 頁(從 - 到) | 183-190 |
| 頁數 | 8 |
| 期刊 | Carbohydrate Research |
| 卷 | 346 |
| 發行號 | 2 |
| DOIs | |
| 出版狀態 | 已出版 - 01 02 2011 |
| 對外發佈 | 是 |