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首页> 外文期刊>American journal of transplantation: official journal of the American Society of Transplantation and the American Society of Transplant Surgeons >Antigen-dependent interactions between regulatory B cells and T cells at the T:B border inhibit subsequent T cell interactions with DCs
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Antigen-dependent interactions between regulatory B cells and T cells at the T:B border inhibit subsequent T cell interactions with DCs

机译:调节B细胞和T细胞之间的抗原依赖性相互作用在T:B边界抑制随后的T细胞与DCS相互作用

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摘要

IL-10+ regulatory B cells (Bregs) inhibit immune responses in various settings. While Bregs appear to inhibit inflammatory cytokine expression by CD4+ T cells and innate immune cells, their reported impact on CD8+ T cells is contradictory. Moreover, it remains unclear which effects of Bregs are direct versus indirect. Finally, the subanatomical localization of Breg suppressive function and the nature of their intercellular interactions remain unknown. Using novel tamoxifen-inducible B cell-specific IL-10 knockout mice, we found that Bregs inhibit CD8+ T cell proliferation and inhibit inflammatory cytokine expression by both CD4+ and CD8+ T cells. Sort-purified Bregs from IL-10-reporter mice were adoptively transferred into wild-type hosts and examined by live-cell imaging. Bregs localized to the T:B border, specifically entered the T cell zone, and made more frequent and longer contacts with both CD4+ and CD8+ T cells than did non-Bregs. These Breg:T cell interactions were antigen-specific and reduced subsequent T:DC contacts. Thus, Bregs inhibit T cells through direct cognate interactions that subsequently reduce DC:T cell interactions.
机译:IL-10 +调节B细胞(BREG)在各种环境中抑制免疫应答。虽然Bregs似乎通过CD4 + T细胞和先天免疫细胞抑制炎症细胞因子表达,但它们报告的对CD8 + T细胞的影响是矛盾的。此外,仍然不清楚Bregs与间接相比的哪种效果。最后,BREG抑制功能​​的脱盲化定位及其细胞间相互作用的性质仍然未知。使用新型制革诱导的B细胞特异性IL-10敲除小鼠,我们发现BREGS抑制CD8 + T细胞增殖并抑制CD4 +和CD8 + T细胞的炎症细胞因子表达。将来自IL-10-Reporter小鼠的分类纯化的坯料用过型宿主进行,并通过活细胞成像检查。本地化为T:B边界的Bregs,具体地进入T细胞区域,并使CD4 +和CD8 + T细胞的更频繁和更长的触点而不是非折叠。这些贫雷格:T细胞相互作用是抗原特异性的,随后的T:DC触点。因此,Bregs通过随后减少DC:T细胞相互作用的直接同源相互作用来抑制T细胞。

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