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滤泡调节性 T 细胞抑制表达颗粒酶 B 的滤泡辅助性 T 细胞的发育。

Follicular regulatory T cells inhibit the development of granzyme B-expressing follicular helper T cells.

机构信息

Department of Microbiology and Immunology, Indiana University School of Medicine, Indianapolis, Indiana, USA.

Indiana University School of Informatics and Computing, Indiana University-Purdue University Indianapolis, Indianapolis, Indiana, USA.

出版信息

JCI Insight. 2019 Aug 22;4(16):128076. doi: 10.1172/jci.insight.128076.

Abstract

T follicular regulatory (TFR) cells are found in the germinal center (GC) response and help shape the antibody (Ab) response. However, the precise role of TFR cells in the GC is controversial. Here, we addressed TFR cell function using mice with impaired TFR cell development (Bcl6-flox/Foxp3-cre, or Bcl6FC mice), mice with augmented TFR cell development (Blimp1-flox/Foxp3-cre, or Blimp1FC mice), and two different methods of immunization. Unexpectedly, GC B cell levels positively correlated with TFR cell levels. Using a gene profiling approach, we found that TFH cells from TFR-deficient mice showed strong upregulation of granzyme B (Gzmb) and other effector CD8+ T cell genes, many of which were Stat4 dependent. The upregulation of cytotoxic genes was the highest in TFH cells from TFR-deficient mice where Blimp1 was also deleted in Foxp3+ regulatory T cells (Bcl6-flox/Prdm1-flox/Foxp3-cre [DKO] mice). Granzyme B- and Eomesodermin-expressing TFH cells correlated with a higher rate of apoptotic GC B cells. Klrg1+ TFH cells from DKO mice expressed higher levels of Gzmb. Our data show that TFR cells repress the development of abnormal cytotoxic TFH cells, and the presence of cytotoxic TFH cells correlates with a lower GC and Ab response. Our data show what we believe is a novel mechanism of action for TFR cells helping the GC response.

摘要

滤泡辅助性 T(Tfh)细胞存在于生发中心(GC)反应中,有助于塑造抗体(Ab)反应。然而,Tfh 细胞在 GC 中的确切作用存在争议。在这里,我们使用 TFR 细胞发育受损的小鼠(Bcl6-flox/Foxp3-cre,或 Bcl6FC 小鼠)、TFR 细胞发育增强的小鼠(Blimp1-flox/Foxp3-cre,或 Blimp1FC 小鼠)以及两种不同的免疫方法来解决 TFR 细胞功能问题。出乎意料的是,GC B 细胞水平与 TFR 细胞水平呈正相关。通过基因谱分析,我们发现 TFR 缺陷小鼠的 TFH 细胞强烈地上调了颗粒酶 B(Gzmb)和其他效应 CD8+T 细胞基因,其中许多基因依赖于 Stat4。在 TFR 缺陷小鼠中,TFH 细胞中的细胞毒性基因上调最为显著,其中 Foxp3+调节性 T 细胞中也缺失了 Blimp1(Bcl6-flox/Prdm1-flox/Foxp3-cre [DKO] 小鼠)。表达颗粒酶 B 和 Eomesodermin 的 TFH 细胞与更高比例的凋亡 GC B 细胞相关。DKO 小鼠的 Klrg1+TFH 细胞表达更高水平的 Gzmb。我们的数据表明,TFR 细胞抑制异常细胞毒性 TFH 细胞的发育,而存在细胞毒性 TFH 细胞与较低的 GC 和 Ab 反应相关。我们的数据显示了 TFR 细胞帮助 GC 反应的一种新的作用机制。

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