皂甙元
差向异构体
立体中心
化学
生物碱
立体化学
有机化学
对映选择合成
医学
病理
催化作用
替代医学
作者
Aneta Baj,Nirawit Kaewnok,Juan A. Rivas‐Loaiza,Magdalena Szymańska,Stanisław Witkowski,Agnieszka Wojtkielewicz,Jacek W. Morzycki
标识
DOI:10.1002/chem.202203314
摘要
Abstract A simple synthesis method of solanidane alkaloids from common steroidal sapogenins was developed. Previously described multi‐step transformations of tigogenin to demissidine (8–12 steps) were shortened to four steps only. The key‐step of the present synthesis was the epimerization at C25 of the lactam intermediate. Different approaches to this reaction, i. e., a classical one via enolate, and a chemoselective umpolung transformation, were thoroughly investigated. The epimerization step is unnecessary if the starting sapogenin has the same configuration at C25 as the target alkaloid because the configuration at C25 (either R or S ) remains intact throughout the synthesis. Thus, the related solanidane alkaloids, 12β‐hydroxy‐25‐ epi ‐demissidine and 5‐ epi ‐demissidine, were synthesized in the three‐step procedure with retention of configuration at this stereogenic center from rockogenin (25 R ‐5α‐sapogenin) or sarsasapogenin (25 S ‐5β‐sapogenin), respectively.
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