Stereospecific synthesis by the sodium salt glycosylation method of halogeno benzimidazole 2'-deoxyribose analogues of the inhibitor of hnRNA synthesis, 5,6-dichloro-1-(beta-D-ribofuranosyl)benzimidazole (DRB).

Z Kazimierczuk, R Stolarski, D Shugar
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引用次数: 8

Abstract

The recently developed stereospecific sodium salt glycosylation procedure has been successfully applied to the synthesis of the beta-D-2'-deoxyribofuranosides of benzimidazole, 5,6-dihalogeno benzimidazoles, and some 2-substituted analogues in high yield. The 5,6-dibromo analogue was obtained by bromination of the parent nucleoside. These have all been characterized by spectroscopic methods, including 1H NMR, which permitted analyses of their solution conformations and comparison with those of the corresponding ribofuranosides. Some biological aspects, including preliminary results on cytotoxicity and antiviral activity, are briefly considered.

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用钠盐糖基化法立体定向合成卤代苯并咪唑2′-脱氧核糖类似物的hnRNA合成抑制剂5,6-二氯-1-(β -d -核呋喃基)苯并咪唑(DRB)。
最近开发的立体定向钠盐糖基化方法已成功地用于合成苯并咪唑、5,6-二卤基苯并咪唑和一些2取代类似物的β -d -2'-脱氧核呋喃苷类化合物,收率较高。通过母体核苷的溴化得到5,6-二溴类似物。这些都通过光谱方法进行了表征,包括1H NMR,可以分析它们的溶液构象,并与相应的核呋喃苷进行比较。一些生物学方面,包括细胞毒性和抗病毒活性的初步结果,简要地考虑。
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