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Transcription Factor IRF4 Dysfunction Affects the Immunosuppressive Function of Treg Cells in Patients with Primary Immune Thrombocytopenia 期刊论文

编号：

16ab6182-ce0a-4cfa-9623-809304f8ecfc
作者：

Tang, Meiwen#^[1]Cheng, Luya(承璐雅)^[1]Li, Feng(李锋)^[1,2]Wu, Boting^[3];Chen, Pu(陈朴)^[4]Zhan, Yanxia(詹延霞)^[1]Hua, Fanli(化范例)^[2]Min, Zhihui^[5];Ke, Yang^[1];Liu, Chanjuan^[1];Yuan, Ling^[1];Sun, Lihua(孙丽华)^[2]Chen, Hao^[6];Ji, Lili(季丽莉)*^[1]Cheng, Yunfeng(程韵枫)*^[1,2,5,7]
语种：

英文
期刊：

BIOMED RESEARCH INTERNATIONAL ISSN：2314-6133 2019 年 2019 卷 ; JUL 10
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摘要：

Background. Th17/Treg balance skews towards Th17 in ITP patient. IRF4 has been highlighted for its close relationship to the immunosuppressive function of Treg cells and the IL-17 synthesis in CD4(+) T cells. This study was aimed at examining the effects of IRF4 to the Th17/Treg cells in patients with ITP. Methods. Treg and Teff cells were isolated from PBMCs of newly diagnosed ITP patients. The percentages of CD4(+)CD25(hi)Foxp3(+)Treg cells and the CD3(+)CD4(+)IL-17(+)Th17 cells were detected by flow cytometry. After being cultured, the supernatants of Tregs were collected for IL-10 concentration test. The IRF4 levels of Tregs were measured. Teffs were cultured alone or with Tregs for 24 hours. Then the supernatants were collected for IL-17 concentration test. The binding intensity of IRF4 to the gene IL-10 in Treg cells was detected by ChIP-qPCR. Metabolic assays for Teffs and Tregs were performed with Agilent Seahorse XF96 Analyzer. Results. The secretion of IL-10 by Tregs was decreased in ITP patients. The intensity of IRF4 binding to IL-10 DNA of Tregs in patients was higher than that of normal controls and Teffs in ITP patients. The expressions of IRF4 of Tregs in ITP patients were remarkably lower than that of healthy controls. The percentage of Th17 cells in healthy controls was significantly increased after IRF4 mRNA silencing. Abnormal metabolism of Treg and Teff cells was found in ITP patients. Conclusion. The skewed ratio of Th17/Treg cells and dysfunction of Treg cells in newly diagnosed ITP patients was at least partly caused by IRF4 dysfunction. The underlying mechanism might be the impact of IRF4 on the metabolism of Treg and Teff cells.
推荐引用方式
GB/T 7714：

Tang Meiwen,Cheng Luya,Li Feng, et al. Transcription Factor IRF4 Dysfunction Affects the Immunosuppressive Function of Treg Cells in Patients with Primary Immune Thrombocytopenia [J].BIOMED RESEARCH INTERNATIONAL,2019,2019.
APA：

Tang Meiwen,Cheng Luya,Li Feng,Wu Boting,&Cheng Yunfeng.(2019).Transcription Factor IRF4 Dysfunction Affects the Immunosuppressive Function of Treg Cells in Patients with Primary Immune Thrombocytopenia .BIOMED RESEARCH INTERNATIONAL,2019.
MLA：

Tang Meiwen, et al. "Transcription Factor IRF4 Dysfunction Affects the Immunosuppressive Function of Treg Cells in Patients with Primary Immune Thrombocytopenia" .BIOMED RESEARCH INTERNATIONAL 2019(2019).
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