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先天性PLZF+CD4+αβT细胞在缺乏Itk的情况下发育并扩增。

Innate PLZF+CD4+ αβ T cells develop and expand in the absence of Itk.

作者信息

Prince Amanda L, Watkin Levi B, Yin Catherine C, Selin Liisa K, Kang Joonsoo, Schwartzberg Pamela L, Berg Leslie J

机构信息

Department of Pathology, University of Massachusetts Medical School, Worcester, MA 01655; and.

National Human Genome Research Institute, National Institutes of Health, Bethesda, MD 20814.

出版信息

J Immunol. 2014 Jul 15;193(2):673-87. doi: 10.4049/jimmunol.1302058. Epub 2014 Jun 13.

Abstract

T cell development in the thymus produces multiple lineages of cells, including innate T cells. Studies in mice harboring alterations in TCR signaling proteins or transcriptional regulators have revealed an expanded population of CD4(+) innate T cells in the thymus that produce IL-4 and express the transcription factor promyelocytic leukemia zinc finger (PLZF). In these mice, IL-4 produced by the CD4(+)PLZF(+) T cell population leads to the conversion of conventional CD8(+) thymocytes into innate CD8(+) T cells resembling memory T cells expressing eomesodermin. The expression of PLZF, the signature invariant NKT cell transcription factor, in these innate CD4(+) T cells suggests that they might be a subset of αβ or γδ TCR(+) NKT cells or mucosal-associated invariant T (MAIT) cells. To address these possibilities, we characterized the CD4(+)PLZF(+) innate T cells in itk(-/-) mice. We show that itk(-/-) innate PLZF(+)CD4(+) T cells are not CD1d-dependent NKT cells, MR1-dependent MAIT cells, or γδ T cells. Furthermore, although the itk(-/-) innate PLZF(+)CD4(+) T cells express αβ TCRs, neither β2-microglobulin-dependent MHC class I nor any MHC class II molecules are required for their development. In contrast to invariant NKT cells and MAIT cells, this population has a highly diverse TCRα-chain repertoire. Analysis of peripheral tissues indicates that itk(-/-) innate PLZF(+)CD4(+) T cells preferentially home to spleen and mesenteric lymph nodes owing to increased expression of gut-homing receptors, and that their expansion is regulated by commensal gut flora. These data support the conclusion that itk(-/-) innate PLZF(+)CD4(+) T cells are a novel subset of innate T cells.

摘要

胸腺中的T细胞发育产生多种细胞谱系,包括天然T细胞。对TCR信号蛋白或转录调节因子发生改变的小鼠的研究表明,胸腺中产生IL-4并表达转录因子早幼粒细胞白血病锌指蛋白(PLZF)的CD4(+)天然T细胞群体有所扩大。在这些小鼠中,CD4(+)PLZF(+) T细胞群体产生的IL-4导致传统的CD8(+)胸腺细胞转变为类似表达eomesodermin的记忆T细胞的天然CD8(+) T细胞。这些天然CD4(+) T细胞中PLZF(标志性的不变NKT细胞转录因子)的表达表明它们可能是αβ或γδ TCR(+) NKT细胞或黏膜相关不变T(MAIT)细胞的一个亚群。为了探究这些可能性,我们对itk(-/-)小鼠中的CD4(+)PLZF(+)天然T细胞进行了特征分析。我们发现itk(-/-)天然PLZF(+)CD4(+) T细胞不是CD1d依赖性NKT细胞、MR1依赖性MAIT细胞或γδ T细胞。此外,尽管itk(-/-)天然PLZF(+)CD4(+) T细胞表达αβ TCR,但它们的发育既不需要β2-微球蛋白依赖性的MHC I类分子,也不需要任何MHC II类分子。与不变NKT细胞和MAIT细胞不同,该群体具有高度多样化的TCRα链库。对周围组织的分析表明,由于肠道归巢受体表达增加,itk(-/-)天然PLZF(+)CD4(+) T细胞优先归巢至脾脏和肠系膜淋巴结,并且它们的扩增受共生肠道菌群调节。这些数据支持了itk(-/-)天然PLZF(+)CD4(+) T细胞是天然T细胞的一个新亚群这一结论。

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