细粒棘球绦虫
生物
免疫系统
免疫学
FOXP3型
先天免疫系统
动物
作者
S. S. Yin,X. Chen,Jin-biao ZHANG,Fei Xu,Hongwei Fang,Jun Hou,Xiaoyang Zhang,Xiangwei Wu,X. Chen
摘要
Summary Cystic echinococcosis ( CE ) caused by the cestode Echinococcus granulosus ( E. granulosus ) is a zoonotic parasitic disease. The effective immune evasion mechanisms of E. granulosus allow it to parasitize its hosts. However, the status of the innate and adaptive immune cells and their contributions to E. granulosus progression remain poorly understood. In this study, we aimed to determine the impact of E. granulosus infection on T cells, NK cell responses and TGF ‐β expression during the early infection phase in BALB /c mice. In E. granulosus infections, there was an increasing tendency in the percentage of CD 4 + CD 25 + T cells and CD 4 + Foxp3 + T cells and peripheral blood TGF ‐β levels and relative expression of the Foxp3 gene. Moreover, there were a decreasing tendency in the percentage of NK cells and NK cell cytotoxicity and the expression of NKG 2D on NK cells. The TGF ‐β1/Smad pathway was activated by E. granulosus in mice. Above results can be reversed by the inhibitor SB ‐525334 (potent activin receptor‐like kinase 5 inhibitor). These results suggest that the TGF ‐β/Smad pathway plays an important role in changes of T‐cell or NK cell responses. These results may contribute to revealing the preliminary molecular mechanisms in establishing hydatid infection.
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