Kyoto Pharmaceutical University , Misasagi, Yamashina, Kyoto 607-8412, Japan.
J Org Chem. 2016 Sep 2;81(17):7471-85. doi: 10.1021/acs.joc.6b01154. Epub 2016 Aug 1.
Pd(II)-catalyzed ring formation of 2,3,5-trisubstituted and 2,3,4,5-tetrasubstituted tetrahydrofurans is described. Oxypalladation of a chiral ε-hydroxy allylic alcohol provides a 5-alkenyltetrahydrofuran ring in excellent yields via a 5-exo-trigonal process. Nine substrates including six secondary allylic alcohols and three primary allylic alcohols with or without an additional secondary hydroxy substituent at the γ-position have been examined. Their structures are restricted by a 2,2,4,4-tetraisopropyl-1,3,5,2,4-trioxadisilocane ring. The stereochemistry of the resulting tetrahydrofuran products was determined by chemical transformation. The reaction mechanism is discussed on the basis of the stereochemical results. The steps in the chiral allylic alcohol directed or the nucleophilic alcohol directed facial selection for the formation of the alkene-Pd(II)-π-complex, the cis-oxypalladation, and a syn-elimination mechanism account for the observed stereochemistry of the reaction.
Pd(II)催化的 2,3,5-三取代和 2,3,4,5-四取代四氢呋喃的环形成反应被描述。通过 5-endo-trig 过程,手性 ε-羟烯丙基醇的氧化钯化以优异的收率提供了 5-烯基四氢呋喃环。包括六个仲烯丙基醇和三个仲烯丙基醇在内的 9 个底物以及三个在 γ-位具有额外的仲羟基取代基的仲烯丙基醇都被研究过。它们的结构受到 2,2,4,4-四异丙基-1,3,5,2,4-四氧代二硅杂环戊烷环的限制。通过化学转化确定了所得四氢呋喃产物的立体化学。根据立体化学结果讨论了反应机理。在形成烯烃-Pd(II)-π-配合物、顺式氧化钯化和 syn-消除过程中,手性烯丙醇导向或亲核醇导向的面选择性步骤解释了反应的观察到的立体化学。
