CD22结合涎苷的改进合成及其在进一步开发有效CD22抑制剂中的应用。

IF 2.7 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Yuki Suganuma, Akihiro Imamura, Hiromune Ando, Makoto Kiso, Hiromu Takematsu, Takeshi Tsubata, Hideharu Ishida
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引用次数: 0

摘要

CD22是一种唾液酸结合免疫球蛋白样凝集素(Siglecs),通过与带有Neu5Ac/Gcα(2→6)Gal序列的聚糖配体相互作用调节B淋巴细胞信号传导。我们已经开发了合成的涎苷GSC-718作为CD22的配体模拟物,并鉴定其为有效的CD22抑制剂。虽然本课题组已经报道了包括GSC-718在内的结合cd22的涎苷类化合物的合成,但遗憾的是该合成路线不适合大规模合成。在这项研究中,我们开发了一种改进的可扩展的合成方法,以1,5-内酰胺的形成为关键步骤。改进后的方法得到在C2位置含有一系列苷元的皂苷。一些以取代苄基残基为苷元的衍生物被发现与小鼠CD22结合,其亲和力与GSC-718相当。本研究中开发的新程序为基于细胞的检测提供了足够数量的唾液皂苷,并将促进寻找具有治疗潜力的有前途的CD22抑制剂。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Improved synthesis of CD22-binding sialosides and its application for further development of potent CD22 inhibitors.

Improved synthesis of CD22-binding sialosides and its application for further development of potent CD22 inhibitors.

CD22, one of the sialic acid-binding immunoglobulin-like lectins (Siglecs), regulates B lymphocyte signaling via its interaction with glycan ligands bearing the sequence Neu5Ac/Gcα(2→6)Gal. We have developed the synthetic sialoside GSC-718 as a ligand mimic for CD22 and identified it as a potent CD22 inhibitor. Although the synthesis of CD22-binding sialosides including GSC-718 has been reported by our group, the synthetic route was unfortunately not suitable for large-scale synthesis. In this study, we developed an improved scalable synthetic procedure for sialosides which utilized 1,5-lactam formation as a key step. The improved procedure yielded sialosides incorporating a series of aglycones at the C2 position. Several derivatives with substituted benzyl residues as aglycones were found to bind to mouse CD22 with affinity comparable to that of GSC-718. The new procedure developed in this study affords sialosides in sufficient quantities for cell-based assays, and will facilitate the search for promising CD22 inhibitors that have therapeutic potential.

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来源期刊
Glycoconjugate Journal
Glycoconjugate Journal 生物-生化与分子生物学
CiteScore
6.00
自引率
3.30%
发文量
63
审稿时长
1 months
期刊介绍: Glycoconjugate Journal publishes articles and reviews on all areas concerned with: function, composition, structure, biosynthesis, degradation, interactions, recognition and chemo-enzymatic synthesis of glycoconjugates (glycoproteins, glycolipids, oligosaccharides, polysaccharides and proteoglycans), biochemistry, molecular biology, biotechnology, immunology and cell biology of glycoconjugates, aspects related to disease processes (immunological, inflammatory, arthritic infections, metabolic disorders, malignancy, neurological disorders), structural and functional glycomics, glycoimmunology, glycovaccines, organic synthesis of glycoconjugates and the development of methodologies if biologically relevant, glycosylation changes in disease if focused on either the discovery of a novel disease marker or the improved understanding of some basic pathological mechanism, articles on the effects of toxicological agents (alcohol, tobacco, narcotics, environmental agents) on glycosylation, and the use of glycotherapeutics. Glycoconjugate Journal is the official journal of the International Glycoconjugate Organization, which is responsible for organizing the biennial International Symposia on Glycoconjugates.
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