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首页> 外文期刊>Australian Journal of Chemistry: A Journal for the Publication of Original Research in All Branches of Chemistry >Assembly of the 1-Azaspiro[5.5]undecane Framework Associated with Perhydrohistrionicotoxin via Electrocyclic Ring-Opening of a Ring-Fused gem-Dichlorocyclopropane and Trapping of the Resulting pi-Allyl Cation by a Tethered,Nitrogen-Centered Nucleophi
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Assembly of the 1-Azaspiro[5.5]undecane Framework Associated with Perhydrohistrionicotoxin via Electrocyclic Ring-Opening of a Ring-Fused gem-Dichlorocyclopropane and Trapping of the Resulting pi-Allyl Cation by a Tethered,Nitrogen-Centered Nucleophi

机译:1-氮杂螺[5.5]十一烷骨架与全氢组氨酸毒素的结合,通过环合的宝石-二氯环丙烷的电环开环并通过以氮为中心的束缚核捕集所得的π-烯丙基阳离子

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摘要

The carbamate-tethered gem-dichlorocyclopropane 27 was prepared,as a mixture of epimers,in ten steps from commercially available beta,gamma-unsaturated nitrile 9.Upon treatment with silver acetate under a range of reaction conditions,compound 27 underwent electrocyclic ring opening to give the corresponding pi-allyl cation that was then trapped by the reaction solvent,chloride ion,and/or acetate ion,and so affording varying mixtures of the chlorocyclohexenes 28,29,30,and/or 31.Sequential treatment of the same substrate with LiHMDS (to generate the conjugate base of this carbamate)then silver tetrafluoroborate afforded the chlorocyclohexadiene 32 as the exclusive product of reaction.No spirocyclization product of the type 3 arising from trapping of the intermediate pi-allyl cation by the tethered carbamate was observed under any of the reaction conditions examined.In contrast,analogous treatment of the more rigid system 38 afforded compound 39 incorporating the 1 -azaspiro[5.5]undecane framework associated with the potent neurotoxin perhydrohistrionicotoxin (2).
机译:氨基甲酸酯系的宝石-二氯环丙烷27是差向异构体的混合物,是从市售的β,γ-不饱和腈9.十步制备的。在一系列反应条件下用乙酸银处理后,化合物27进行开环电得到相应的pi-烯丙基阳离子,然后被反应溶剂,氯离子和/或乙酸根离子截留,从而提供氯环己烷28、29、30和/或31的不同混合物。用LiHMDS(生成该氨基甲酸酯的共轭碱),然后四氟硼酸银提供了氯环己二烯32作为反应的唯一产物。没有观察到在束缚氨基甲酸酯的作用下,中间的π-烯丙基阳离子被束缚的氨基甲酸酯捕获而引起的3型螺环化产物。相比之下,对较刚性系统38的类似处理得到包含1-azaspiro [5.5]十一烷的化合物39与强效神经毒素过氢组织毒素相关的框架(2)。

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