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Versatile procedure for asymmetric and orthogonal protection of symmetric polyamines and its advantages for solid phase synthesis

机译:对称多胺不对称和正交保护的通用方法及其在固相合成中的优势

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摘要

To date, many polyamine syntheses are carried out on solid phase to allow the generation of biologically active polyamine conjugates and libraries of natural product analogs. The synthesis of compounds and libraries, which derive from a symmetric polyamine building block such as spermine requires asymmetric and orthogonal protection of the symmetric polyamine. For this purpose we have established a novel Aloc- and Nosyl-protection group strategy, which displays several advantages. Solution phase synthesis and an easy workup reveals high yield of the asymmetrically and orthogonally protected polyamine. Asymmetric protection prevents cross-linking of the resin, and sequential deprotection can occur on highly acid and base labile resins without cleavage of the linker. Finally, it tolerates the elongation and modification of the symmetric polyamine backbone with several functional groups by conventional Fukuyama-alkylation. The suitability of this protection group strategy was shown by the first solid phase synthesis of the philanthotoxin-analog HO359b.
机译:迄今为止,许多多胺合成是在固相上进行的,以产生具有生物活性的多胺缀合物和天然产物类似物的文库。衍生自对称多胺结构单元(如精胺)的化合物和库的合成需要对称多胺的不对称和正交保护。为此,我们建立了一种新颖的Aloc和Nosyl保护基策略,该策略显示了许多优点。溶液相合成和简单的后处理揭示了不对称和正交保护的多胺的高产率。不对称保护可防止树脂发生交联,并且在高度酸和碱不稳定的树脂上可以发生连续的脱保护反应,而不会裂解连接基。最后,通过常规的福山烷基化,它可以容忍带有多个官能团的对称多胺骨架的伸长和修饰。 philanthotoxin-analog HO359b的第一个固相合成表明了这种保护基策略的适用性。

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