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首页> 外文期刊>Scandinavian journal of immunology. >Ageing down-modulates liver inflammatory immune responses to schistosome infection in mice.
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Ageing down-modulates liver inflammatory immune responses to schistosome infection in mice.

机译:衰老下调小鼠对血吸虫感染的肝炎性免疫反应。

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Ageing is associated with several alterations in the immune system. Our aim in this study was to compare the development of immunity to Schistosoma mansoni infection in young versus aged C57Bl/6 mice using the liver as the main organ to evaluate pathological alterations and immune responses. In the acute phase, young mice had large liver granulomas with fibrosis and inflammatory cells. Chronic phase in young animals was associated with immunomodulation of granulomas that became reduced in size and cellular infiltrate. On the other hand, aged animals presented granulomas of smaller sizes already in the acute phase. Chronic infection in these mice was followed by no alteration in any of the inflammatory parameters in the liver. In concert with this finding, there was an increase in activated CD4+ T, CD19+ B and NK liver cells in young mice after infection whereas old mice had already higher frequencies of activated B, NK and CD4+ T liver cells and infection does not change these frequencies. After infection, liver production of inflammatory and regulatory cytokines such as IFN-gamma, IL-4 and IL-10 increased in young but not in old mice that had high levels of IL-4 and IL-10 regardless of their infection status. Our data suggest that the unspecific activation status of the immune system in aged mice impairs inflammatory as well as regulatory immune responses to S. mansoni infection in the liver, where major pathological alterations and immunity are at stage. This poor immune reactivity may have a beneficial impact on disease development.
机译:衰老与免疫系统的多种变化有关。我们在这项研究中的目的是比较以肝脏为主要器官评估病理改变和免疫反应的年轻和老年C57Bl / 6小鼠对曼氏血吸虫感染的免疫力。在急性期,年轻小鼠患有大型肝肉芽肿,并伴有纤维化和炎性细胞。幼年动物的慢性期与肉芽肿的免疫调节有关,肉芽肿的大小和细胞浸润都减少了。另一方面,老年动物在急性期已经出现了较小尺寸的肉芽肿。在这些小鼠中的慢性感染之后,肝脏中的任何炎症参数都没有改变。与这一发现相一致的是,感染后的年轻小鼠中活化的CD4 + T,CD19 + B和NK肝细胞增加,而老龄小鼠已经具有较高的活化B,NK和CD4 + T肝细胞频率,感染不会改变这些频率。感染后,无论感染状况如何,幼鼠肝脏中产生的炎性和调节性细胞因子(如IFN-γ,IL-4和IL-10)的产量均会增加,但在高龄小鼠中却不会增加。我们的数据表明,老年小鼠免疫系统的非特异性激活状态会损害肝脏对曼氏沙门氏菌感染的炎症反应以及调节性免疫反应,而肝脏的主要病理改变和免疫作用尚处于阶段。这种不良的免疫反应性可能对疾病的发展产生有益的影响。

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