慢性小肠蠕虫感染对肠上皮通透性的调节。

IF 3.2 4区 医学 Q3 CELL BIOLOGY
Thomas C Mules, Jeffry S Tang, Francesco Vacca, Bibek Yumnam, Alfonso Schmidt, Brittany Lavender, Kate Maclean, Sophia-Louise Noble, Craig Waugh, Roel van Ginkel, Mali Camberis, Graham Le Gros, Stephen Inns
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引用次数: 0

摘要

肠道上皮细胞层的通透性增加与多种肠道和肠道外疾病的发病机制和持续存在有关。有人建议用控制剂量的蠕虫(如人类钩虫)感染人类(称为钩虫疗法),以此治疗许多相同的疾病。蠕虫会诱导宿主发生免疫调节变化,从而降低上皮细胞的通透性,这被认为是蠕虫治疗疾病的一种潜在机制。尽管如此,慢性蠕虫感染对上皮通透性的影响仍不清楚。本研究利用慢性感染肠道蠕虫Heligmosomoides polygyrus揭示了感染过程中肠道紧密连接蛋白表达和上皮通透性的变化。在急性感染阶段(感染后 1 周),观察到肠道上皮通透性增加。与这一发现相一致的是,空肠 claudin-2 上调,而三尖杉蛋白下调。相比之下,在慢性感染阶段(感染后 6 周),结肠 claudin-1 上调,上皮通透性降低。重要的是,这项研究还调查了实验性感染人类钩虫(Necator americanus)的小部分人群上皮通透性的变化。研究表明,小肠通透性在急性感染期(感染后 8 周)呈上升趋势,而结肠和整个肠道的通透性在慢性感染期(感染后 24 周)呈下降趋势,这表明人类和小鼠的上皮反应是一致的。总之,我们的研究结果表明了慢性蠕虫感染期间上皮通透性的动态变化,并为利用慢性蠕虫感染治疗疾病提供了另一种可信的机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Modulation of intestinal epithelial permeability by chronic small intestinal helminth infections

Modulation of intestinal epithelial permeability by chronic small intestinal helminth infections

Increased permeability of the intestinal epithelial layer is linked to the pathogenesis and perpetuation of a wide range of intestinal and extra-intestinal diseases. Infecting humans with controlled doses of helminths, such as human hookworm (termed hookworm therapy), is proposed as a treatment for many of the same diseases. Helminths induce immunoregulatory changes in their host which could decrease epithelial permeability, which is highlighted as a potential mechanism through which helminths treat disease. Despite this, the influence of a chronic helminth infection on epithelial permeability remains unclear. This study uses the chronically infecting intestinal helminth Heligmosomoides polygyrus to reveal alterations in the expression of intestinal tight junction proteins and epithelial permeability during the infection course. In the acute infection phase (1 week postinfection), an increase in intestinal epithelial permeability is observed. Consistent with this finding, jejunal claudin-2 is upregulated and tricellulin is downregulated. By contrast, in the chronic infection phase (6 weeks postinfection), colonic claudin-1 is upregulated and epithelial permeability decreases. Importantly, this study also investigates changes in epithelial permeability in a small human cohort experimentally challenged with the human hookworm, Necator americanus. It demonstrates a trend toward small intestinal permeability increasing in the acute infection phase (8 weeks postinfection), and colonic and whole gut permeability decreasing in the chronic infection phase (24 weeks postinfection), suggesting a conserved epithelial response between humans and mice. In summary, our findings demonstrate dynamic changes in epithelial permeability during a chronic helminth infection and provide another plausible mechanism by which chronic helminth infections could be utilized to treat disease.

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来源期刊
Immunology & Cell Biology
Immunology & Cell Biology 医学-免疫学
CiteScore
7.50
自引率
2.50%
发文量
98
审稿时长
4-8 weeks
期刊介绍: The Australasian Society for Immunology Incorporated (ASI) was created by the amalgamation in 1991 of the Australian Society for Immunology, formed in 1970, and the New Zealand Society for Immunology, formed in 1975. The aim of the Society is to encourage and support the discipline of immunology in the Australasian region. It is a broadly based Society, embracing clinical and experimental, cellular and molecular immunology in humans and animals. The Society provides a network for the exchange of information and for collaboration within Australia, New Zealand and overseas. ASI members have been prominent in advancing biological and medical research worldwide. We seek to encourage the study of immunology in Australia and New Zealand and are active in introducing young scientists to the discipline.
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