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在固相上进行阿马多里修饰肽的位点特异性合成。

Site-specific synthesis of Amadori-modified peptides on solid phase.

作者信息

Frolov Andrej, Singer David, Hoffmann Ralf

机构信息

Bioanalytics, Center for Biotechnology and Biomedicine, Faculty of Chemistry and Mineralogy, University of Leipzig, Deutscher Platz 5, 04103 Leipzig, Germany.

出版信息

J Pept Sci. 2006 Jun;12(6):389-95. doi: 10.1002/psc.739.

Abstract

Glycation of peptides and proteins is a slow chemical reaction of reducing sugars modifying the amino groups. The first intermediates of this nonenzymatic glycosylation are the Amadori products that can undergo further chemical reactions, finally leading to advanced glycation end products (AGEs). The formation of AGEs was not only linked to aging of tissues and organs in general but also to several diseases such as diabetes mellitus and Alzheimer's disease. Because of the importance of these modifications and their potential use as diagnostic markers, a global postsynthetic approach on solid phase was developed. The peptides were synthesized by Fmoc/(t)Bu-chemistry, with the lysine residue to be modified being protected with the very acid-labile methyltrityl group. Incubation of the peptides with D-glucose in DMF at elevated temperatures resulted in product yields of 35%. Neighboring residues with bulky protecting groups reduced the yields only slightly. The major by-products were the unmodified peptide and an oxidation product. Whereas the unmodified peptide eluted before the glycated peptide, all other by-products eluted later in RP-HPLC, allowing simple purification.

摘要

肽和蛋白质的糖基化是还原糖修饰氨基的缓慢化学反应。这种非酶糖基化的最初中间体是阿马多里产物,其可进一步发生化学反应,最终生成晚期糖基化终产物(AGEs)。AGEs的形成不仅与组织和器官的整体衰老有关,还与多种疾病相关,如糖尿病和阿尔茨海默病。由于这些修饰的重要性及其作为诊断标志物的潜在用途,人们开发了一种基于固相的全局合成后方法。肽通过Fmoc/(t)Bu化学法合成,待修饰的赖氨酸残基用对酸非常不稳定的三苯甲基保护。在高温下于N,N -二甲基甲酰胺(DMF)中将肽与D -葡萄糖孵育,产物产率为35%。带有庞大保护基团的相邻残基仅使产率略有降低。主要副产物是未修饰的肽和一种氧化产物。未修饰的肽在糖基化肽之前洗脱,而所有其他副产物在反相高效液相色谱(RP - HPLC)中较晚洗脱,从而实现简单纯化。

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