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使用简单模型系统研究糖缀合物中的新型环状结构。

Investigation of novel cyclic structure in glycoconjugate using a simple model system.

机构信息

Analytical Research and Development, BioTherapeutics Pharmaceutical Sciences, Pfizer, Inc., 875 Chesterfield Parkway West, Chesterfield, MO, 63017, United States.

Analytical Research and Development, BioTherapeutics Pharmaceutical Sciences, Pfizer, Inc., 875 Chesterfield Parkway West, Chesterfield, MO, 63017, United States.

出版信息

Carbohydr Res. 2020 Sep;495:108103. doi: 10.1016/j.carres.2020.108103. Epub 2020 Jul 23.

DOI:10.1016/j.carres.2020.108103
PMID:32807353
Abstract

Bacterial capsular polysaccharide protein conjugates are a major class of vaccines for preventing severe bacterial infections. The conjugation of a polysaccharide to a carrier protein is critical for inducing adaptive immune response in healthy humans. Due to the high molecular mass and extensive structural heterogeneity of the glycoconjugate, the underlying sugar linkages and polypeptide site selectivity of the conjugation reaction are not well characterized and understood. Here, we report a model conjugation study using a monosaccharide and a synthetic peptide to investigate the fundamental reductive amination chemistry, which is one of the most commonly utilized conjugation strategies for glycoconjugate vaccines. We identified a cyclic tertiary amine linkage as the primary conjugation linkage for monosaccharides containing dialdehydes. Such linkage is previously not well-recognized by the glycoconjugate vaccine field. Our study has provided insights into this commonly used, yet complex conjugation chemistry and will benefit the design of future protein-polysaccharide-based vaccines.

摘要

细菌荚膜多糖蛋白缀合物是预防严重细菌感染的主要疫苗类别。多糖与载体蛋白的缀合对于诱导健康人群的适应性免疫反应至关重要。由于糖缀合物的高分子质量和广泛的结构异质性,缀合反应的糖键和多肽位点选择性的基础尚未得到很好的表征和理解。在这里,我们使用单糖和合成肽报告了一项模型缀合研究,以研究还原性胺化化学,这是糖缀合物疫苗最常用的缀合策略之一。我们确定了环状叔胺键作为含有二醛的单糖的主要缀合键。这种键合以前没有被糖缀合物疫苗领域很好地识别。我们的研究提供了对这种常用但复杂的缀合化学的深入了解,将有益于未来基于蛋白质-多糖的疫苗的设计。

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