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猪幽门螺杆菌通过两种模式与人及猪胃粘蛋白和糖脂上的碳水化合物结合。

Helicobacter suis binding to carbohydrates on human and porcine gastric mucins and glycolipids occurs via two modes.

机构信息

a Department of Medical Biochemistry and Cell Biology , Institute of Biomedicine, Sahlgrenska Academy, University of Gothenburg , Gothenburg , Sweden.

b Department of Pathology , Bacteriology and Avian Diseases, Ghent University , Belgium.

出版信息

Virulence. 2018 Dec 31;9(1):898-918. doi: 10.1080/21505594.2018.1460979.

Abstract

Helicobacter suis colonizes the stomach of most pigs and is the most prevalent non-Helicobacter pylori Helicobacter species found in the human stomach. In the human host, H. suis contributes to the development of chronic gastritis, peptic ulcer disease and MALT lymphoma, whereas in pigs it is associated with gastritis, decreased growth and ulcers. Here, we demonstrate that the level of H. pylori and H. suis binding to human and pig gastric mucins varies between individuals with species dependent specificity. The binding optimum of H. pylori is at neutral pH whereas that of H. suis has an acidic pH optimum, and the mucins that H. pylori bind to are different than those that H. suis bind to. Mass spectrometric analysis of mucin O-glycans from the porcine mucin showed that individual variation in binding is reflected by a difference in glycosylation; of 109 oligosaccharide structures identified, only 14 were present in all examined samples. H. suis binding to mucins correlated with glycans containing sulfate, sialic acid and terminal galactose. Among the glycolipids present in pig stomach, binding to lactotetraosylceramide (Galβ3GlcNAcβ3Galβ4Glcβ1Cer) was identified, and adhesion to Galβ3GlcNAcβ3Galβ4Glc at both acidic and neutral pH was confirmed using other glycoconjugates. Together with that H. suis bound to DNA (used as a proxy for acidic charge), we conclude that H. suis has two binding modes: one to glycans terminating with Galβ3GlcNAc, and one to negatively charged structures. Identification of the glycan structures H. suis interacts with can contribute to development of therapeutic strategies alternative to antibiotics.

摘要

猪源螺杆菌定植于大多数猪的胃中,是人类胃中最常见的非幽门螺杆菌属螺杆菌。在人类宿主中,猪源螺杆菌导致慢性胃炎、消化性溃疡病和黏膜相关淋巴组织(MALT)淋巴瘤的发生,而在猪中则与胃炎、生长不良和溃疡相关。在这里,我们证明了人源和猪源胃黏蛋白中幽门螺杆菌和猪源螺杆菌的结合水平因物种而异,具有物种特异性。幽门螺杆菌的结合最佳 pH 值为中性,而猪源螺杆菌的结合最佳 pH 值为酸性,且幽门螺杆菌结合的黏蛋白与猪源螺杆菌结合的黏蛋白不同。对猪黏蛋白 O-糖链的质谱分析表明,结合的个体差异反映了糖基化的差异;在所检查的 109 个寡糖结构中,只有 14 个存在于所有检查样本中。猪源螺杆菌与黏蛋白的结合与含有硫酸盐、唾液酸和末端半乳糖的聚糖有关。在猪胃中存在的糖脂中,鉴定到与乳糖四糖基神经酰胺(Galβ3GlcNAcβ3Galβ4Glcβ1Cer)结合,并且在酸性和中性 pH 下使用其他糖缀合物证实了与 Galβ3GlcNAcβ3Galβ4Glc 的粘附。结合猪源螺杆菌与 DNA 结合(用作酸性电荷的替代物),我们得出结论,猪源螺杆菌具有两种结合模式:一种与 Galβ3GlcNAc 末端的聚糖结合,另一种与带负电荷的结构结合。鉴定猪源螺杆菌相互作用的聚糖结构可以为开发替代抗生素的治疗策略做出贡献。

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