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强效盐皮质激素19-去甲醛固酮的合成。

Synthesis of 19-noraldosterone, a potent mineralocorticoid.

作者信息

Harnik M, Kashman Y, Cojocaru M, Rosenthal T, Morris D J

出版信息

J Steroid Biochem. 1986 Jun;24(6):1163-9. doi: 10.1016/0022-4731(86)90378-x.

Abstract

19-Noraldosterone has been prepared for biological re-evaluation through an extension of a recent synthesis of 19-hydroxyaldosterone: 21-hydroxy-6 beta,19-epoxy-4-pregnene-3,20-dion-20-ethylene ketal-18,11 beta-lactone (1a) was acetylated and then reduced with zinc-acetic acid-isopropanol to the 19-ol 2b. Treatment with sodium acetate transposed the double bond into conjugation, and 2a thus obtained was oxidized with pyridinium chlorochromate to the 19-oxo compound 3. Decarbonylation to the 19-nor lactone 4 was effected by heating with alkali. Protection of the C-3 carbonyl was achieved by ketalization and the resulting mixture of the 5-ene and 5(10)-ene ketals 5 was reduced with DIBAH to the corresponding mixture of the hemiacetals 6. Acid hydrolysis of the latter afforded 19-noraldosterone (7), accompanied by the 18,21-anhydro ketal 8. 19-Noraldosterone in the solid state exists in the cyclic form 7b, which appears to be also the predominant isomer present under conditions of mass spectrometry. [1H]NMR indicates that in chloroform 19-noraldosterone exists mostly as an equilibrium mixture of structures 7a and 7b. Sodium periodate oxidation furnished the gamma-etiolactone 9, confirming the 17 beta configuration in 7.

摘要

通过扩展最近对19-羟基醛固酮的合成方法,已制备出19-去甲醛固酮用于生物学重新评估:将21-羟基-6β,19-环氧-4-孕烯-3,20-二酮-20-乙烯缩酮-18,11β-内酯(1a)进行乙酰化,然后用锌-乙酸-异丙醇还原为19-醇2b。用乙酸钠处理使双键共轭移位,如此得到的2a用氯铬酸吡啶鎓氧化为19-氧代化合物3。通过与碱加热进行脱羰反应得到19-去甲内酯4。通过缩酮化保护C-3羰基,所得的5-烯和5(10)-烯缩酮5的混合物用二异丁基氢化铝还原为相应的半缩醛6的混合物。后者经酸水解得到19-去甲醛固酮(7),同时伴有18,21-脱水缩酮8。固态的19-去甲醛固酮以环状形式7b存在,这似乎也是质谱条件下存在的主要异构体。[1H]NMR表明,在氯仿中19-去甲醛固酮主要以结构7a和7b的平衡混合物形式存在。高碘酸钠氧化得到γ-乙内酰脲9,证实了7中17β构型。

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