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(25R)-和(25S)-皂苷元中C-22的差向异构化

Epimerization of C-22 in (25R)- and (25S)-sapogenins.

作者信息

Viñas-Bravo Omar, Merino-Montiel Penélope, Romero-López Anabel, Montiel-Smith Sara, Meza-Reyes Socorro, Meléndez Francisco J, Sandoval-Ramírez Jesús

机构信息

Instituto de Química Aplicada, Universidad del Papaloapan, Circuito Central # 200, Colonia Parque Industrial, Tuxtepec, Oax. 68301, Mexico.

Facultad de Ciencias Químicas, Benemérita Universidad Autónoma de Puebla, Ciudad Universitaria, Puebla, Pue. 72570, Mexico.

出版信息

Steroids. 2015 Jan;93:60-7. doi: 10.1016/j.steroids.2014.10.004. Epub 2014 Nov 20.

Abstract

Most of the naturally occurring steroidal sapogenins (C-23 non-substituted frameworks), possess an R configuration at the spiro C-22 center. Their C-22 epimers have become important targets in biological research. This paper describes a procedure to obtain 22S-spirostans from 22R-sapogenins and pseudosapogenin skeletons, without affecting the chirality at either C-25 or C-20. An optimal way to synthesize the pair of C-22 stereoisomers of 23-acetyldiosgenin is also reported. The latter was obtained from a 22,26-epoxycholestane or from 23-acetylfurostene compounds.

摘要

大多数天然存在的甾体皂苷元(C-23未取代骨架)在螺环C-22中心具有R构型。它们的C-22差向异构体已成为生物学研究中的重要目标。本文描述了一种从22R-皂苷元和假皂苷元骨架获得22S-螺旋甾烷的方法,且不影响C-25或C-20处的手性。还报道了合成23-乙酰基薯蓣皂苷元C-22立体异构体对的最佳方法。后者可从22,26-环氧胆甾烷或23-乙酰基呋甾烯化合物获得。

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