首页> 美国卫生研究院文献>PLoS Neglected Tropical Diseases >Intra-Subtype Variation in Enteroadhesion Accounts for Differences in Epithelial Barrier Disruption and Is Associated with Metronidazole Resistance in Blastocystis Subtype-7
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Intra-Subtype Variation in Enteroadhesion Accounts for Differences in Epithelial Barrier Disruption and Is Associated with Metronidazole Resistance in Blastocystis Subtype-7

机译:肠粘连的亚型内变异解释上皮屏障破坏的差异并与Blastocystis亚型7的甲硝唑耐药性有关。

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摘要

Blastocystis is an extracellular, enteric pathogen that induces intestinal disorders in a range of hosts including humans. Recent studies have identified potential parasite virulence factors in and host responses to this parasite; however, little is known about Blastocystis-host attachment, which is crucial for colonization and virulence of luminal stages. By utilizing 7 different strains of the parasite belonging to two clinically relevant subtypes ST-4 and ST-7, we investigated Blastocystis-enterocyte adhesion and its association with parasite-induced epithelial barrier disruption. We also suggest that drug resistance in ST-7 strains might result in fitness cost that manifested as impairment of parasite adhesion and, consequently, virulence. ST-7 parasites were generally highly adhesive to Caco-2 cells and preferred binding to intercellular junctions. These strains also induced disruption of ZO-1 and occludin tight junction proteins as well as increased dextran-FITC flux across epithelial monolayers. Interestingly, their adhesion was correlated with metronidazole (Mz) susceptibility. Mz resistant (Mzr) strains were found to be less pathogenic, owing to compromised adhesion. Moreover, tolerance of nitrosative stress was also reduced in the Mzr strains. In conclusion, the findings indicate that Blastocystis attaches to intestinal epithelium and leads to epithelial barrier dysfunction and that drug resistance might entail a fitness cost in parasite virulence by limiting entero-adhesiveness. This is the first study of the cellular basis for strain-to-strain variation in parasite pathogenicity. Intra- and inter-subtype variability in cytopathogenicity provides a possible explanation for the diverse clinical outcomes of Blastocystis infections.
机译:胚泡是一种细胞外的肠道病原体,可在包括人类在内的许多宿主中诱发肠道疾病。最近的研究已经确定了这种寄生虫中潜在的寄生物毒力因子并对其做出了反应。然而,关于囊胚-宿主附着的知识鲜为人知,这对于管腔阶段的定殖和毒力至关重要。通过利用属于两种临床相关亚型ST-4和ST-7的7种不同菌株的寄生虫,我们研究了囊胚芽孢杆菌-肠癌细胞的粘附及其与寄生虫诱导的上皮屏障破坏的关系。我们还建议,ST-7菌株的耐药性可能会导致健身成本降低,表现为寄生虫粘附力下降,进而导致毒力下降。 ST-7寄生虫通常对Caco-2细胞具有很高的粘附力,并与细胞间连接具有较好的结合力。这些菌株还诱导了ZO-1和occludin紧密连接蛋白的破坏,并增加了跨上皮单层的右旋糖酐-FITC通量。有趣的是,它们的粘附性与甲硝唑(Mz)敏感性相关。由于粘附力受损,发现耐Mz的(Mz r )菌株致病性较低。此外,Mz r 菌株的亚硝化胁迫耐受性也降低。总之,研究结果表明,囊胚芽孢菌附着在肠上皮上并导致上皮屏障功能障碍,而耐药性可能会通过限制肠黏附性而导致寄生虫毒力的产生。这是首次研究寄生虫致病性之间的变异的细胞基础。细胞内致病性的亚型间和亚型间变异性为囊藻感染的多种临床结果提供了可能的解释。

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