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Effect of prebiotic oligosaccharides on enteropathogenic Escherichia coli adherence.

机译:益生元寡糖对肠致病性大肠杆菌粘附的影响。

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摘要

Antiadhesion therapy has been found to be a very promising means to prevent and treat infections in the respiratory, urinary, and gastrointestinal tract. Despite the considerable research interest in antiadhesives, relatively little is known about the ability of commercial dietary oligosaccharides, such as prebiotics, to inhibit pathogen adherence. The goal of this research was to determine if commercially available prebiotic oligosaccharides could function as antiadhesive agents against enteropathogenic E. coli (EPEC).; To investigate the ability of prebiotics to inhibit EPEC adherence, inhibition assays were performed by comparing adherence rates of EPEC on HEp-2 and Caco-2 cells in the presence of galactooligosaccharides (GOS), inulin, fructooligosaccharides, lactulose, or raffinose. These data showed that GOS significantly reduced binding of EPEC more than the other prebiotics tested. In addition, binding inhibition by GOS was shown to be dose-dependent and saturable at 16 mg/ml. Microscopic analyses indicated that GOS also reduced the number of EPEC per microcolony and the total number of microcolonies per infected cell.; Both therapeutic and prophylactic GOS treatments were also examined. GOS was unable to displace previously adhered EPEC, but could prevent EPEC adherence when administered prior to infection. Additionally, GOS did not affect EPEC autoaggregation. To determine if GOS was inhibiting adherence at a molecular level, the expression of BfpA, a bundle forming pili protein involved in localized adherence, was examined. GOS did not affect BfpA expression indicating that adherence inhibition was not due to the absence of this adhesin.; To further examine the role of EPEC adhesins in GOS-mediated adherence inhibition, adherence assays using HEp-2 and Caco-2 cell lines were performed using isogenic EPEC mutants. In general, GOS did not affect the adherence of strains lacking BfpA, suggesting that GOS may interfere specifically with BfpA-receptor interactions rather than with other potential EPEC adhesins and their receptors. These results show that commercial prebiotics, particularly GOS, directly inhibit the adherence of E. coli, and provides evidence that these agents may be used as antiadhesives against pathogens in both humans and animals.
机译:已经发现抗粘连疗法是预防和治疗呼吸道,泌尿道和胃肠道感染的非常有前途的手段。尽管在抗粘剂方面有相当大的研究兴趣,但对于商业饮食中的低聚糖(如益生元)抑制病原体粘附的能力知之甚少。这项研究的目的是确定市售的益生元寡糖是否可以作为抗肠病原性大肠杆菌(EPEC)的抗粘剂。为了研究益生元抑制EPEC粘附的能力,通过比较在低聚半乳糖(GOS),菊粉,低聚果糖,乳果糖或棉子糖存在下EPEC对HEp-2和Caco-2细胞的粘附率来进行抑制试验。这些数据表明,GOS比其他测试的益生元更能显着降低EPEC的结合。此外,GOS的结合抑制作用是剂量依赖性的,在16 mg / ml时可饱和。显微分析表明,GOS还减少了每个微菌落的EPEC数量和每个感染细胞的微菌落总数。还检查了GOS的治疗性和预防性治疗。 GOS无法取代以前粘附的EPEC,但在感染前给药可阻止EPEC粘附。此外,GOS不会影响EPEC自动聚合。为了确定GOS是否在分子水平上抑制粘附,检查了BfpA(参与局部粘附的成束菌毛蛋白)的表达。 GOS不影响BfpA的表达,表明粘附抑制不是由于该粘附素的缺乏。为了进一步检查EPEC粘附素在GOS介导的粘附抑制中的作用,使用同基因EPEC突变体进行了使用HEp-2和Caco-2细胞系的粘附测定。通常,GOS不会影响缺乏BfpA的菌株的粘附,这表明GOS可能会特异性干扰BfpA-受体相互作用,而不是其他潜在的EPEC粘附素及其受体。这些结果表明,商品益生元,特别是GOS,直接抑制了大肠杆菌的粘附,并提供了证据,证明这些试剂可用作人和动物体内病原体的抗粘剂。

著录项

  • 作者

    Shoaf, Kari.;

  • 作者单位

    The University of Nebraska - Lincoln.;

  • 授予单位 The University of Nebraska - Lincoln.;
  • 学科 Agriculture Food Science and Technology.; Biology Microbiology.
  • 学位 Ph.D.
  • 年度 2007
  • 页码 179 p.
  • 总页数 179
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 农产品收获、加工及贮藏;微生物学;
  • 关键词

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