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Polar Dibenzocyclooctynes for Selective Labeling of Extracellular Glycoconjugates of Living Cells

机译:极性二苯并吲哚Clooctynes用于皮细胞的细胞外血糖缀合物的选择性标记

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摘要

Although strain-promoted alkyne-azide cycloadditions (SPAAC) have found wide utility in biological and material sciences, the low polarity and limited water solubility of commonly used cyclooctynes represents a serious shortcoming. To address this problem, an efficient synthetic route has been developed for highly polar sulfated dibenzocyclooctynylamides (S-DIBO) by a Friedel-Crafts alkylation of 1,2-bis(3-methoxyphenyl)ethylamides with trichlorocyclopropenium cation followed by a controlled hydrolysis of the resulting dichlorocyclopropenes to give bis(3-methoxyphenyl)cyclooctacyclopropenones, which were subjected to methoxy group removal of the phenols, O-sulfation, and photochemical unmasking of the cyclopropenone moiety. Accurate rate measurements of the reaction of benzyl azide with various dibenzylcyclooctyne derivatives demonstrated that aromatic substitution and the presence of the amide function had only a marginal impact on the rate constants. Biotinylated S-DIBO >8 was successfully used for labeling azido-containing glycoconjugates of living cells. Furthermore, it was found that the substitution pattern of the dibenzylcyclooctynes influences subcellular location and in particular it has been shown that DIBO derivative >4 can enter cells thereby labeling intra- and extracellular azido-modified glycoconjugates, whereas S-DIBO >8 cannot pass the cell membrane and therefore is ideally suited for selective labeling of cell surface molecules. The ability to selectively label cell surface molecules will yield unique opportunities for glycomic analysis and the study of glycoprotein trafficking.
机译:虽然应变促进的炔氧化物环加成(SPAAC)在生物和物质科学中发现了广泛的效用,但常用的CycloCodynes的低极性和有限的水溶性代表了严重的缺点。为了解决这个问题,通过用三氯环丙烯酰胺的Friedel-Crafts烷基化与三氯环丙烯酰胺的Friedel-Crafts烷基化,然后进行三氯环丙烯酰基阳离子,然后对其进行了高抗体硫酸化二苯并苯并苯并辛酰基酰胺(S-Dibo),然后进行了一种有效的合成途径。得到二氯环丙烯,得到双(3-甲氧基苯基)环辛酰基丙酮,其对甲氧基除去酚,O-硫化和光化学揭露环烯酮部分的光化学。苄基叠氮化物与各种二苄基环偶联衍生物的准确率测量表明芳族取代和酰胺功能的存在对速率常数仅产生边缘撞击。生物素化的S-Dibo > 8℃,用于标记含有含有含氮杂的活细胞的糖缀合物。此外,发现二苄基环菌的替代图案影响亚细胞位置,特别是已经表明,Dibo衍生物<强> 4℃可以进入细胞,从而标记细胞内和细胞外α-改性的糖凝胶缀合物,而S- Dibo > 8 不能通过细胞膜,因此非常适合选择性标记细胞表面分子。选择性标记细胞表面分子的能力将为糖类分析和糖蛋白贩运的研究产生独特的机会。

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