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糖辅助的复杂寡糖糖肽连接:范围与局限性

Sugar-assisted glycopeptide ligation with complex oligosaccharides: scope and limitations.

作者信息

Bennett Clay S, Dean Stephen M, Payne Richard J, Ficht Simon, Brik Ashraf, Wong Chi-Huey

机构信息

Department of Chemistry, The Scripps Research Institute, 10550 North Torrey Pines Road, La Jolla, California 92037, USA.

出版信息

J Am Chem Soc. 2008 Sep 10;130(36):11945-52. doi: 10.1021/ja8010513. Epub 2008 Aug 13.

Abstract

We have previously shown sugar-assisted ligation (SAL) to be a useful method for the convergent construction of glycopeptides. However to date SAL has only been carried out on systems where the thiol auxiliary is attached to a monosaccharide. For SAL to be truly applicable to the construction of fully elaborated glycopeptides and glycoproteins, it must be possible to carry out the reaction when the thiol auxiliary is attached to more elaborate sugars, as these are frequently what are observed in nature. Here we examine the effects of glycosylation at C-3, C-4, and C-6 of the C-2 auxiliary-containing glycan. Model glycopeptides where synthesized chemoenzymatically and reacted with peptide thioesters used in our previous work. These studies reveal that SAL is sensitive to extended glycosylation on the auxiliary-containing sugar. While it is possible to carry out SAL with extended glycosylation at C-4 and C-6, the presence of glycosylation at C-3 prevents the ligation from occurring. Additionally, with glycosylation at C-4 the ligation efficiency is affected by the identity of the N-terminal AA, while the nature of the C-terminal residue of the peptide thioester does not appear to affect ligation efficiency. These studies provide useful guidelines in deciding when it is appropriate to use SAL in the synthesis of complex glycopeptides and glycoproteins and how to choose ligation junctions for optimal yield.

摘要

我们之前已经证明糖辅助连接(SAL)是一种用于糖肽汇聚式构建的有用方法。然而,迄今为止,SAL仅在硫醇辅助基团连接到单糖的体系中进行。为了使SAL真正适用于构建完全精细的糖肽和糖蛋白,当硫醇辅助基团连接到更复杂的糖上时必须能够进行该反应,因为这些糖在自然界中经常出现。在这里,我们研究了含C-2辅助基团聚糖的C-3、C-4和C-6位糖基化的影响。通过化学酶法合成模型糖肽,并使其与我们之前工作中使用的肽硫酯反应。这些研究表明,SAL对含辅助基团糖上的延长糖基化敏感。虽然在C-4和C-6位进行延长糖基化时可以进行SAL,但C-3位存在糖基化会阻止连接反应的发生。此外,对于C-4位糖基化,连接效率受N端氨基酸身份的影响,而肽硫酯C端残基的性质似乎不影响连接效率。这些研究为决定何时在合成复杂糖肽和糖蛋白时使用SAL以及如何选择连接位点以获得最佳产率提供了有用的指导方针。

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