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The Crystal Structure of Shiga Toxin Type 2 with Bound Disaccharide Guides the Design of a Heterobifunctional Toxin Inhibitor

机译:带有绑定的二糖的志贺毒素2型的晶体结构指导异双功能毒素抑制剂的设计。

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摘要

Shiga toxin type 2 (Stx2a) is clinically most closely associated with enterohemorrhagic E. coli O157:H7-mediated hemorrhagic colitis that sometimes progresses to hemolytic-uremic syndrome. The ability to express the toxin has been acquired by other Escherichia coli strains, and outbreaks of food poisoning have caused significant mortality rates as, for example, in the 2011 outbreak in northern Germany. Stx2a, an AB5 toxin, gains entry into human cells via the glycosphingolipid receptor Gb3. We have determined the first crystal structure of a disaccharide analog of Gb3 bound to the B5 pentamer of Stx2a holotoxin. In this Gb3 analog, α-GalNAc replaces the terminal α-Gal residue. This co-crystal structure confirms previous inferences that two of the primary binding sites identified in the B5 pentamer of Stx1 are also functional in Stx2a. This knowledge provides a rationale for the synthesis and evaluation of heterobifunctional antagonists for E. coli toxins that target Stx2a. Incorporation of GalNAc Gb3 trisaccharide in a heterobifunctional ligand with an attached pyruvate acetal, a ligand for human amyloid P component, and conjugation to poly[acrylamide-co-(3-azidopropylmethacrylamide)] produced a polymer that neutralized Stx2a in a mouse model of Shigatoxemia.
机译:志贺毒素2型(Stx2a)在临床上与肠出血性大肠杆菌O157:H7介导的出血性结肠炎密切相关,有时会发展为溶血性尿毒症综合征。其他大肠杆菌菌株已经获得了表达毒素的能力,而且食物中毒的爆发已导致很高的死亡率,例如,2011年德国北部的爆发。 Stx2a,一种AB5毒素,通过糖鞘脂受体Gb3进入人体细胞。我们已经确定了与Stx2a全毒素的B5五聚体结合的Gb3二糖类似物的第一个晶体结构。在该Gb3类似物中,α-GalNAc取代了末端α-Gal残基。这种共晶体结构证实了先前的推论,即在Stx1的B5五聚体中鉴定出的两个主要结合位点在Stx2a中也起作用。该知识为合成和评估靶向Stx2a的大肠杆菌毒素的异双功能拮抗剂提供了理论依据。在异双功能配体中将GalNAc Gb3三糖与附着的丙酮酸缩醛,人淀粉样蛋白P组分的配体结合,并与聚[丙烯酰胺-co-(3-叠氮基丙基甲基丙烯酰胺)结合]产生了一种聚合物,该聚合物在志贺毒素血症小鼠模型中中和了Stx2a。 。

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