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Total Synthesis and Biological Evaluation of Ipomoeassin F and Its Unnatural 11R-Epimer

机译:Ipomoeassin F及其非天然11R-表异构体的全合成及生物学评价

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摘要

Ipomoeassin F, a macrolide glycoresin containing an embedded disaccharide, possesses potent in vitro antitumor activity with an unknown mechanism of function. It inhibits tumor cell growth with single-digit nanomolar IC50 values, superior to many clinical chemotherapeutic drugs. To facilitate translation of its bioactivity into protein function for drug development, we report here a new synthesis for the gram-scale production of ipomoeassin F (3.8% over 17 linear steps) from commercially-available starting materials. The conformation-controlled subtle reactivity differences of the hydroxyl groups in carbohydrates were utilized to quickly construct the disaccharide core, which, along with judicial selection of protecting groups, made the current synthesis very efficient. The same strategy was also applied to the smooth preparation of the 11R-epimer of ipomoeassin F for the first time. Cytotoxicity assays demonstrated the crucial role of the natural 11S configuration. In addition, cell cycle analyses and apoptosis assays on ipomoeassin F and/or its epimer were conducted. This work has laid a solid ground for understanding the medicinal potential of the ipomoeassin family of glycolipids in the future.
机译:Ipomoeassin F是一种含有内嵌二糖的大环内酯糖脂,具有强大的体外抗肿瘤活性,但其功能机制尚不清楚。它以一位数纳摩尔的IC50值抑制肿瘤细胞的生长,优于许多临床化学治疗药物。为了促进将其生物活性转化为蛋白质功能以开发药物,我们在这里报告了一种新的合成方法,用于从商业上可用的起始原料克级生产ipomoeassin F(在17个线性步骤中为3.8%)。利用糖中羟基的构象控制的微妙反应性差异来快速构建二糖核心,再加上对保护基的合理选择,使得目前的合成非常有效。相同的策略也首次应用于ipomoeassin F的11R-受体的顺利制备。细胞毒性试验证明了天然11S构型的关键作用。另外,对ipomoeassin F和/或其差向异构体进行细胞周期分析和凋亡测定。这项工作为理解未来ipomoeassin糖脂家族的医学潜力奠定了坚实的基础。

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