Division of Organic Chemistry, National Chemical Laboratory, Pune, 411008, India.
Org Biomol Chem. 2009 Aug 21;7(16):3300-7. doi: 10.1039/b907007a. Epub 2009 Jun 19.
A highly divergent route to a variety of quinolizidine alkaloids is described. The enantiomeric precursors and utilized for the synthesis of these alkaloids were constructed stereospecifically from the PET cyclization of the corresponding acetylene tethered alpha-trimethylsilyl amine moieties and , respectively, both of which were synthesised from D-ribose. The polyhydroxy quinolizidine alkaloid was found to be a selective inhibitor of alpha-galactosidase with Ki 83.9 microM. The amine analogs , and are found to be selective and potent inhibitors of alpha-glucosidase with Ki 28, 120 and 140 microM, respectively.
描述了一种通往各种喹诺里西啶生物碱的高度差异途径。这些生物碱的对映体前体是通过相应的乙炔键合的α-三甲基硅基胺部分的 PET 环化,分别从 D-核糖立体特异性构建的,这两种物质都可以从 D-核糖合成。多羟基喹诺里西啶生物碱被发现是α-半乳糖苷酶的选择性抑制剂,Ki 为 83.9μM。胺类似物、和被发现是α-葡萄糖苷酶的选择性和有效抑制剂,Ki 分别为 28、120 和 140μM。
