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首页> 外文期刊>Immunology: An Official Journal of the British Society for Immunology >The roles of antigen-specificity, responsiveness to transforming growth factor-beta and antigen-presenting cell subsets in tumour-induced expansion of regulatory T cells.
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The roles of antigen-specificity, responsiveness to transforming growth factor-beta and antigen-presenting cell subsets in tumour-induced expansion of regulatory T cells.

机译:抗原特异性,对转化生长因子-β和抗原呈递细胞亚群的响应在肿瘤诱导的调节性T细胞扩增中的作用。

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摘要

In this study we investigated the impact of several factors on the expansion of natural regulatory T (nTreg) cells by tumours, including antigen specificity, transforming growth factor-beta (TGF-beta) signalling and the antigen-presenting cell subsets responsible for expansion. We found that antigen non-specific expansion of nTreg cells is tumour cell line-dependent. Although both antigen-specific and non-specific pathways can contribute to expansion, the migration of activated nTreg cells to tumour tissues is strictly antigen-dependent. Intact TGF-beta signalling on nTreg cells is also essential for tumour-induced expansion. Finally, for stimulation of resting antigen-specific CD4 T cells, CD11c(+) cells purified from tumour-draining lymph nodes were more potent than CD11b(+) cells, suggesting that dendritic cells are the key antigen-presenting cell subset involved in cross-presentation of tumour antigens. This study not only provides an in vivo system in which cross-talk between nTreg cells and tumours can be explored but also reveals novel aspects of tumour immune evasion.
机译:在这项研究中,我们调查了多种因素对自然调节T(nTreg)细胞受肿瘤扩增的影响,包括抗原特异性,转化生长因子β(TGF-beta)信号传导和负责扩展的抗原呈递细胞亚群。我们发现nTreg细胞的抗原非特异性扩增是肿瘤细胞系依赖性的。尽管抗原特异性和非特异性途径均可促进扩增,但活化的nTreg细胞向肿瘤组织的迁移严格依赖抗原。 nTreg细胞上完整的TGF-β信号对于肿瘤诱导的扩增也是必不可少的。最后,对于刺激静息的抗原特异性CD4 T细胞,从引流肿瘤的淋巴结中纯化的CD11c(+)细胞比CD11b(+)细胞更有效,这表明树突状细胞是参与交叉的关键抗原呈递细胞亚群。 -肿瘤抗原的呈递。这项研究不仅提供了一种体内系统,可以探索nTreg细胞与肿瘤之间的串扰,而且还揭示了肿瘤免疫逃避的新方面。

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