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首页> 外文期刊>Chemistry: A European journal >Complex biohopanoids synthesis: Efficient anchoring of ribosyl Subunits onto a C-30 hopane
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Complex biohopanoids synthesis: Efficient anchoring of ribosyl Subunits onto a C-30 hopane

机译:复杂的生物偶极合成:有效地锚固核糖基亚基在C-30血糖上

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Bacteriohopanoids represent a particularly important series of triterpenoids, widely distributed in bacteria. One of the common features of these pentacyclic hopanepolyols is the presence of an extended non-terpenoid and polyhydroxylated side chain attached to the triterpenic moiety through a CC bond. The biological function of biohopanoids also has to be addressed when one considers the broad diversity in both structures and functionalities found in the side chain. Moreover, the stereochemistries of some biohopanoids are still unconfirmed, due to the lack of synthetic methods to prepare them. In this study we describe an efficient methodology for the formation of the C-C bond between the C-30-hopane component and C-5-polyhydroxylated carbohydrates through the use of a hopanyllithium intermediate, which has enabled us to synthesize several biohopanoid derivatives. We also report the first synthesis of hopanepentol bearing an additional hydroxy group at position C31.
机译:噬菌体代表了一系列特别重要的三萜系列,广泛分布在细菌中。 这些五环磷酸酚浮选的一个共同特征是通过CC键合附着于三萜部分的延长的非萜类化合物和多羟基化侧链。 当一个人认为在侧链中发现的结构和功能的广泛多样化时,也必须解决生物偶极药的生物学功能。 此外,由于缺乏制备它们的合成方法,一些生物偶极药物的立体化学仍然是未经证实的。 在该研究中,我们通过使用寄生铝锂中间体来描述C-30-欧洲丙烷组分和C-5-多羟基化碳化碳水化合物之间的C-C键的高效方法,这使得我们使我们能够合成几种生物偶极衍生物。 我们还报告了在C31位置携带另外的羟基的Hopanepentol的第一个合成。

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