首页> 外文期刊>European Journal of Immunology >A matter of timing: early, not chronic phase intestinal nematode infection restrains control of a concurrent enteric protozoan infection.
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A matter of timing: early, not chronic phase intestinal nematode infection restrains control of a concurrent enteric protozoan infection.

机译:的时间:早,不是慢性阶段肠道线虫感染抑制控制并发肠的原生动物感染。

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摘要

Infections with parasitic worms are often long lasting and associated with modulated immune responses. We analyzed the influence of the nematode Heligmosomoides polygyrus bakeri dwelling in the small intestine on concurrent protozoan infection with Eimeria falciformis residing in the cecum. To dissect the effects of a nematode infection in the early versus chronic phase, we infected animals with E. falciformis 6 or 28 days post H. p. bakeri infection. Only a concurrent early nematode infection led to an increased replication of the protozoan parasite, whereas a chronic worm infection had no influence on the control of E. falciformis. Increased protozoan replication correlated with the reduced production of IFN-gamma, IL-12/23, CCL4, CXCL9 and CXCL10, reduced migration of T cells and increased expression of Foxp3 at the site of protozoan infection. This was accompanied by a stronger nematode-specific Th2 response in gut-draining LN. Protection of mice against challenge infections with the protozoan parasite was not altered. Hence, the detrimental effect of a nematode infection on the control of a concurrent protozoan infection is transient and occurs only in the narrow time window of the early phase of infection.
机译:感染寄生虫通常长持久和调节免疫响应。居住在并发小肠原生动物感染艾美球虫属falciformis居住在盲肠。线虫感染的早期和慢性阶段,我们受感染动物大肠falciformis 6或28天邮报惠普bakeri感染。并发早期线虫感染导致增加的复制原生动物寄生虫,而慢性蠕虫感染没有影响大肠falciformis的控制。原生动物复制与减少生产IFN-gamma IL-12/23,亚兰,CXCL9CXCL10, T细胞的迁移和减少Foxp3的表达增加的站点原生动物感染。更强的nematode-specific Th2反应gut-draining LN。挑战与原生动物寄生虫感染没有改变。线虫感染的控制并发是瞬态和原生动物感染只发生在狭窄的时间窗口感染的早期阶段。

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