首页> 美国卫生研究院文献>Human Vaccines Immunotherapeutics >A multi-epitope vaccine CTB-UE relieves Helicobacter pylori-induced gastric inflammatory reaction via up-regulating microRNA-155 to inhibit Th17 response in C57/BL6 mice model
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A multi-epitope vaccine CTB-UE relieves Helicobacter pylori-induced gastric inflammatory reaction via up-regulating microRNA-155 to inhibit Th17 response in C57/BL6 mice model

机译:多表位疫苗CTB-UE通过上调microRNA-155抑制C57 / BL6小鼠模型中的Th17反应来缓解幽门螺杆菌引起的胃炎反应

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摘要

Vaccination is an effective mean of preventing infectious diseases, including those caused by Helicobacter pylori. Th17 cell responses are critical for the pathogenesis of Helicobacter pylori infection. In view of Th17 responses to multi-epitope vaccine CTB-UE, the IL-17 production in antiserum was examined. CTB-UE immunization decreased IL-17 production, implying that Th17 responses may be inhibited. Furthermore, IL-17 aggravated GES-1 cell injury induced by H. pylori SS1; In contrast, CTB-UE antiserum could alleviate this cell injury, which suggesting that CTB-UE can protect GES-1 cell infected with H. pylori SS1 by inhibiting Th17 responses. Treatment of mice with CTB-UE significantly reduced the H. pylori burden and inflammation in the stomach. On the other hand, the production of IL-17 in the stomach in H. pylori-infected mice was increased; but the production of IL-17 in the stomach was decreased after treatment with CTB-UE. Furthermore, the expression of microRNA-155 in gastric tissue was significantly up-regulated. The results suggested that CTB-UE could relieve the H. pylori-induced gastric inflammatory reaction via up-regulating microRNA-155 to inhibit Th17 responses, implying that the microRNA-155/IL-17 pathway was involved. Further study is required to elucidate the relationship between miRNA-155 and IL-17. We found that the production of IL-17 was significantly increased after the expression of miRNA-155 being down-regulated; however, the production of IL-17 was significantly decreased after the expression of miRNA-155 being upregulated.
机译:疫苗接种是预防包括幽门螺杆菌引起的传染病的有效手段。 Th17细胞反应对于幽门螺杆菌感染的发病机制至关重要。鉴于Th17对多表位疫苗CTB-UE的反应,检查了抗血清中IL-17的产生。 CTB-UE免疫降低了IL-17的产生,暗示Th17反应可能受到抑制。此外,IL-17加重了幽门螺杆菌SS1诱导的GES-1细胞损伤。相反,CTB-UE抗血清可以减轻这种细胞损伤,这表明CTB-UE可以通过抑制Th17反应来保护感染幽门螺杆菌SS1的GES-1细胞。用CTB-UE治疗小鼠可显着降低幽门螺杆菌负担和胃部炎症。另一方面,幽门螺杆菌感染的小鼠的胃中IL-17的产生增加。但是用CTB-UE治疗后,胃中IL-17的产生减少了。此外,microRNA-155在胃组织中的表达明显上调。结果提示,CTB-UE可以通过上调microRNA-155抑制Th17反应来缓解幽门螺杆菌引起的胃部炎症反应,这暗示了microRNA-155 / IL-17通路的参与。需要进一步的研究来阐明miRNA-155和IL-17之间的关系。我们发现,miRNA-155的表达下调后,IL-17的产生显着增加。然而,miRNA-155的表达上调后,IL-17的产生显着降低。

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