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An attempted approach to the tricyclic core of haliclonin A:Structural elucidation of the final product by 2D NMR 被引量:1

An attempted approach to the tricyclic core of haliclonin A:Structural elucidation of the final product by 2D NMR
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摘要 We describe the design and execution of a novel synthetic route to the tricyclic core of haliclonin A,a tetracyclic marine natural product.The approach features Bachi's thiol-medicated free radical cyclization of alkenyl isocyanide to build the bridged ring system,and ring-closing metathesis(RCM) reaction to form the macrocycle.Execution of the synthetic plan ultimately resulted in a diazatricyclic compound.By means of 2D NMR techniques,the structure of this compound was revealed to an unexpected product 8.Analysis of the synthetic pathways allowed concluding that the unexpected product is a result of an "unexpected" migration of olefinic bond during dioxolanation of the 2-cyclohexenone derivative 7.This investigation also resulted in a concise construction of the functionalized hexahydro-1H-isoindole-1,5(4H)-dione 12 and the macrocyclic tricyclic ring system 8. We describe the design and execution of a novel synthetic route to the tricyclic core of haliclonin A,a tetracyclic marine natural product.The approach features Bachi's thiol-medicated free radical cyclization of alkenyl isocyanide to build the bridged ring system,and ring-closing metathesis(RCM) reaction to form the macrocycle.Execution of the synthetic plan ultimately resulted in a diazatricyclic compound.By means of 2D NMR techniques,the structure of this compound was revealed to an unexpected product 8.Analysis of the synthetic pathways allowed concluding that the unexpected product is a result of an "unexpected" migration of olefinic bond during dioxolanation of the 2-cyclohexenone derivative 7.This investigation also resulted in a concise construction of the functionalized hexahydro-1H-isoindole-1,5(4H)-dione 12 and the macrocyclic tricyclic ring system 8.
出处 《Chinese Chemical Letters》 SCIE CAS CSCD 2017年第6期1176-1181,共6页 中国化学快报(英文版)
基金 the National Natural Science Foundation of China(No.21472153) the National Basic Research Program(973 Program)of China(No.2010CB833200) the SKL of Xiamen University(No.201509) the Program for Changjiang Scholars and Innovative Research Team in University of Ministry of Education,China,for financial support
关键词 2D NMR Ring closing metathesis Macrocycles Lactams Structure revision Cyclization 2D NMR Ring closing metathesis Macrocycles Lactams Structure revision Cyclization
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