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首页> 外文期刊>The Journal of Antibiotics: An International Journal >Synthetic studies of the spirocyclic cyclohexene part of versipelostatin, a novel GRP78/Bip molecular chaperone downregulator
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Synthetic studies of the spirocyclic cyclohexene part of versipelostatin, a novel GRP78/Bip molecular chaperone downregulator

机译:新型GRP78 / Bip分子伴侣下调剂versipelostatin螺环环己烯部分的合成研究

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摘要

The spirocyclic part consisting of an -acylated tetronic acid and a multisubstituted cyclohexene embedded in versipelostatin, a novel GRP78/Bip molecular chaperone downregulator, has been synthesized in enantiomerically pure form. The asymmetric synthesis of the targeted spiro4.5-1-oxa-7-decen-2,4-dione derivative was characterized by (1) stereoselective allylation at the -carbon of methylmalonate diester, in which one carboxylic acid was esterified with a D-glucose-derived chiral template, (2) construction of the tetrasubstituted cyclohexenone substructure by high-yielding ring-closing metathesis and (3) stereoselective construction of the spirocyclic tetronic acid part starting from the cyclohexenone obtained as the ring-closing metathesis product.
机译:已经由对映体纯形式合成了螺环部分,该螺环部分由嵌入在versipelostatin中的酰基化的tetronic酸和多取代的环己烯组成,这是一种新型的GRP78 / Bip分子伴侣下调剂。靶向的spiro4.5-1-oxa-7-decen-2,4-dione衍生物的不对称合成的特征在于(1)在丙二酸二甲酯的-碳上进行立体选择性烯丙基化,其中一种羧酸被D酯化-葡萄糖衍生的手性模板,(2)通过高产率的闭环复分解反应构建四取代的环己烯酮亚结构,以及(3)从作为闭环复分解产物的环己烯酮开始的螺环tetronic酸部分的立体选择性构建。

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