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通过结合构象滤波器和结合位点图谱鉴定异种反应性抗体中优先的碳水化合物结合模式。

Identification of preferred carbohydrate binding modes in xenoreactive antibodies by combining conformational filters and binding site maps.

机构信息

Monash Institute of Pharmaceutical Sciences, Monash University, Parkville, VIC 3052, Australia.

出版信息

Glycobiology. 2010 Jun;20(6):724-35. doi: 10.1093/glycob/cwq022. Epub 2010 Feb 22.

Abstract

Carbohydrates are notoriously flexible molecules. However, they have an important role in many biochemical processes as specific ligands. Understanding how carbohydrates are recognized by other biological macromolecules (usually proteins) is therefore of considerable scientific value. Interfering with carbohydrate-protein interactions is a potentially useful strategy in combating a range of disease states, as well as being of critical importance in facilitating allo- and xenotransplantation. We have devised an in silico protocol for analyzing carbohydrate-protein interactions. In this study, we have applied the protocol to determine the structures of alphaGal-terminating carbohydrate antigens in complex with a panel of xenoreactive antibodies. The most important feature of the binding modes is the fixed conformation of the Galbeta(1,4)Glc/GlcNAc linkage across all of the binding modes. The preferred conformation of the terminal Galalpha(1,3)Gal linkage varies depending on the antibody binding site topography, although it is possible that some of the antibodies studied recognize more than one Galalpha(1,3)Gal conformation. The binding modes obtained indicate that each antibody uses distinct mechanisms in recognizing the target antigens.

摘要

碳水化合物是众所周知的灵活分子。然而,作为特定的配体,它们在许多生化过程中起着重要作用。因此,了解碳水化合物如何被其他生物大分子(通常是蛋白质)识别具有相当大的科学价值。干扰碳水化合物-蛋白质相互作用是对抗一系列疾病状态的一种潜在有用的策略,同时对于促进同种异体和异种移植也至关重要。我们设计了一种用于分析碳水化合物-蛋白质相互作用的计算方案。在这项研究中,我们应用该方案来确定与一组异种反应性抗体结合的αGal 末端碳水化合物抗原的结构。结合模式的最重要特征是在所有结合模式中 Galβ(1,4)Glc/GlcNAc 键的固定构象。末端 Galα(1,3)Gal 键的优选构象取决于抗体结合位点的拓扑结构,尽管研究中的一些抗体可能识别不止一种 Galα(1,3)Gal 构象。获得的结合模式表明,每种抗体都使用不同的机制来识别靶抗原。

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