Department of Chemistry, National Taiwan Normal University , 88, Sec. 4, Tingchow Road, Taipei 11677, Taiwan, R.O.C.
Org Lett. 2016 Feb 19;18(4):688-91. doi: 10.1021/acs.orglett.5b03663. Epub 2016 Feb 3.
An unprecedented organocatalytic enantioselective vinylogous Michael addition/Henry cyclization cascade is presented for the synthesis of highly substituted tetrahydrofluoren-9-ones 3 employing novel 1,3-indandione-derived pronucleophiles 1a-g and nitroalkenes 2. Following a very simple protocol, a wide range of products were obtained in good to excellent yields and with excellent enantioinduction (43-98% yield, up to 98% ee). The reaction proceeded with excellent diastereocontrol despite the simultaneous generation of four stereogenic centers. Surprisingly, when 2-(1-phenylethylidene)-1H-indandione (1h) was used as a pronucleophile, no cyclization was observed, and only Michael addition adducts 4a-x were furnished in very good yields and excellent enantioselectivities.
提出了一种前所未有的有机催化对映选择性乙烯基迈克尔加成/亨利环化级联反应,用于合成高度取代的四氢芴-9-酮 3,采用新型 1,3-茚二酮衍生的亲核试剂 1a-g 和硝基烯烃 2。按照非常简单的方案,在良好到优秀的收率和优异的对映选择性(43-98%收率,最高 98%ee)下,得到了广泛的产物。尽管同时生成了四个立体中心,但反应具有极好的非对映选择性控制。令人惊讶的是,当 2-(1-苯亚乙基)-1H-茚二酮(1h)用作亲核试剂时,没有观察到环化,仅以非常好的收率和优异的对映选择性得到迈克尔加成加合物 4a-x。
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