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首页> 外文期刊>Arthritis and Rheumatism >Dichotomous response to transforming growth factor beta after T cell receptor activation by naive CD4+ T cells from DBA/1 mice: enhanced retinoic acid receptor-related orphan nuclear receptor gammat expression yet reduced FoxP3 expression.

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Dichotomous response to transforming growth factor beta after T cell receptor activation by naive CD4+ T cells from DBA/1 mice: enhanced retinoic acid receptor-related orphan nuclear receptor gammat expression yet reduced FoxP3 expression.

机译：DBA / 1小鼠的幼稚CD4 + T细胞激活T细胞受体后对转化生长因子β的二分反应：增强的视黄酸受体相关的孤儿核受体gammat表达，但FoxP3表达降低。

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OBJECTIVE: To investigate the molecular mechanism for biased interleukin-17 (IL-17) production by DBA/1 CD4+ T cells upon T cell receptor (TCR) and transforming growth factor beta (TGFbeta) stimulation. METHODS: Purified naive CD4+ T cells were stimulated with anti-CD3/CD28 under Th1, Th2, Th17, and induced T regulatory (iTreg) cell conditions. Cytokine production was assayed by intracellular staining and enzyme-linked immunosorbent assay. Expression of transcription factors was determined by reverse transcription-polymerase chain reaction, flow cytometry, and immunoblotting techniques. RESULTS: Naive CD4+ T cells from DBA/1 mice produced more IL-17 under Th17 cell polarizing conditions as compared with those from C57BL/6 or BALB/c mice. Further investigation revealed no difference among the strains in terms of CD4+ T cell survival, upstream TCR signaling, or CD69 expression or in the phosphorylation of STAT-3 and expression of suppressor of cytokine signaling 3 that positively or negatively regulate IL-17 cell production. However, DBA/1 CD4+ T cells expressed increased levels of retinoic acid-related orphan receptor gammat (RORgammat). Furthermore, under iTreg cell polarizing conditions, DBA/1 CD4+ T cells showed a strikingly reduced level of FoxP3 expression. When interferon-gamma and IL-4 were blocked, FoxP3 expression increased but remained lower in DBA/1 CD4+ T cells following exposure to TGFbeta as compared with C57BL/6 CD4+ T cells. Moreover, DBA/1 CD4+ T cells showed reduced phosphorylation of Smad2 and Smad3 under both Th17 and iTreg cell polarizing conditions. CONCLUSION: These results indicate that naive CD4+ T cells from DBA/1 mice have a dichotomous response to TGFbeta: enhanced RORgammat, yet reduced FoxP3, up-regulation. This observation may help to elucidate the branch point of TGFbeta signaling that leads to skewed Th17, but reduced iTreg, cell differentiation.

机译：目的：探讨DBA / 1 CD4 + T细胞在T细胞受体（TCR）和转化生长因子β（TGFbeta）刺激下产生白细胞介素17（IL-17）的分子机制。方法：在Th1，Th2，Th17和诱导的T调节（iTreg）细胞条件下，用抗CD3 / CD28刺激纯化的天然CD4 + T细胞。通过细胞内染色和酶联免疫吸附测定法测定细胞因子的产生。通过逆转录-聚合酶链反应，流式细胞仪和免疫印迹技术确定转录因子的表达。结果：与C57BL / 6或BALB / c小鼠相比，DBA / 1小鼠的幼稚CD4 + T细胞在Th17细胞极化条件下产生更多的IL-17。进一步的研究表明，菌株之间在CD4 + T细胞存活率，上游TCR信号传导或CD69表达或STAT-3的磷酸化以及细胞因子信号传导抑制剂3的表达方面均无差异，这些因子正向或负向调节IL-17细胞的产生。但是，DBA / 1 CD4 + T细胞表达的视黄酸相关孤儿受体gammat（RORgammat）的水平增加。此外，在iTreg细胞极化条件下，DBA / 1 CD4 + T细胞的FoxP3表达水平显着降低。当干扰素-γ和IL-4被阻断时，与C57BL / 6 CD4 + T细胞相比，暴露于TGFbeta后DBA / 1 CD4 + T细胞中FoxP3表达增加，但仍然较低。此外，DBA / 1 CD4 + T细胞在Th17和iTreg细胞极化条件下均显示Smad2和Smad3的磷酸化降低。结论：这些结果表明，来自DBA / 1小鼠的幼稚CD4 + T细胞对TGFbeta有二分法反应：RORgammat增强，而FoxP3降低，上调。该观察结果可能有助于阐明TGFbeta信号传导的分支点，该分支点导致偏斜的Th17，但降低了iTreg细胞分化。

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《Arthritis and Rheumatism》 |2011年第1期|共9页
作者
Morita Y; Ismail DM; Elkon KB; Chu CQ;
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正文语种 eng
中图分类免疫性疾病;
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1. Dichotomous response to transforming growth factor beta after T cell receptor activation by naive CD4+ T cells from DBA/1 mice: enhanced retinoic acid receptor-related orphan nuclear receptor gammat expression yet reduced FoxP3 expression. [J] . Morita Y, Ismail DM, Elkon KB, Arthritis and Rheumatism . 2011,第1期

机译：DBA / 1小鼠的幼稚CD4 + T细胞激活T细胞受体后对转化生长因子β的二分反应：增强的视黄酸受体相关的孤儿核受体gammat表达，但FoxP3表达降低。
2. AT-Rich-Interactive Domain-Containing Protein 5A Functions as a Negative Regulator of Retinoic Acid Receptor-Related Orphan Nuclear Receptor gammat-Induced Th17 Cell Differentiation [J] . Yukari Saito, Shin-ichiro Kagami, Yoshie Sanayama, Arthritis and Rheumatism . 2014,第5期

机译：富含AT的相互作用域蛋白5A作为视黄酸受体相关的孤儿核受体gammat诱导Th17细胞分化的负调节剂。
3. Induction of latency-associated peptide (transforming growth factor-beta(1)) expression on CD4+ T cells reduces Toll-like receptor 4 ligand-induced tumour necrosis factor-alpha production in a transforming growth factor-beta-dependent manner. [J] . Boswell S, Sharif S, Alisa A, Immunology: An Official Journal of the British Society for Immunology . 2011,第3期

机译：在CD4 + T细胞上诱导潜伏期相关肽（转化生长因子-β（1））表达以转化生长因子-β依赖的方式降低了Toll样受体4配体诱导的肿瘤坏死因子-α的产生。
4. Culturing and detection of gene expression of transforming growth factor beta type Ⅱ receptor expressing progenitor cells on textile scaffolds fabricated from resorbable PLLA [C] . Harshini Ramakrishna, Ting He, Tieshi Li, World biomaterials congress . 2016

机译：可吸收的PLLA制成的纺织支架上转化生长因子βⅡ型受体表达祖细胞基因表达的培养和检测
5. Transforming growth factor-beta1 activation and transforming growth factor-beta receptor 2 expression levels in the regulation of the TGF-beta signaling pathway. [D] . Rojas, Andres. 2008

机译：在调节TGF-beta信号通路中转化生长因子-beta1激活和转化生长因子-beta受体2的表达水平。
6. Dichotomous response to TGF-β after TCR activation by naïve CD4+ T cells from DBA/1 mice: enhanced RORγt yet reduced Foxp3 expression [O] . Yoshiaki Morita, Doaa M. Ismail, Keith B. Elkon, -1

机译：通过DBA / 1小鼠的NaïveCD4+ T细胞TCR活化后对TGF-β的二分反应：增强的RORγT但减少Foxp3表达
7. Dichotomous response to transforming growth factor β after T cell receptor activation by naive CD4+ T cells from DBA/1 mice: Enhanced retinoic acid receptor-related orphan nuclear receptor γt expression yet reduced FoxP3 expression [O] . Yoshiaki Morita, Doaa M. Ismail, Keith B. Elkon, 2010

机译：通过DBA / 1小鼠的幼稚CD4 + T细胞T细胞受体激活后转化生长因子β的二分反应：增强的视黄酸受体相关孤儿核受体γT表达尚未减少FoxP3表达

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