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白细胞介素-7是人类早期T细胞发育中的关键生长因子。

Interleukin-7 is a critical growth factor in early human T-cell development.

作者信息

Plum J, De Smedt M, Leclercq G, Verhasselt B, Vandekerckhove B

机构信息

Department of Clinical Chemistry, Microbiology, and Immunology, University Hospital of Ghent, Belgium.

出版信息

Blood. 1996 Dec 1;88(11):4239-45.

PMID:8943859
Abstract

Highly purified human CD34+ fetal liver stem cells differentiate to mature T cells when seeded in vitro into isolated fetal thymic lobes of severe combined immunodeficient (SCID) mice followed by fetal thymus organ culture (FTOC). Here, this chimeric human-mouse FTOC was used to address the role of interleukin-7 (IL-7) and of the alpha chain of the IL-7 receptor (IL-7R alpha) in early human T-cell development. We report that addition of either the monoclonal antibody (MoAb) M25, which neutralizes both human and mouse IL-7, or the MoAb M21, which recognizes and blocks exclusively the human high-affinity alpha-chain of the IL-7R, results in a profound reduction in human thymic cellularity. Analysis of lymphoid subpopulations indicates that a highly reduced number of cells undergo maturation from CD34+ precursor cells toward CD4+CD3-CD1+ progenitor cells and subsequently toward CD4+CD8+ thymocytes. Our results reveal a critical role for IL-7 during early human thymocyte development, and may explain the absence or highly reduced levels of T cells in patients with X-linked SCID. The molecular defect in these patients has been shown to be a mutation in the gamma chain of the IL-2R. Although this gamma chain is not only present in the IL-2R, but also forms an essential part of other cytokine receptors, including IL-4, IL-7, IL-9, IL-13, and IL-15, the T-cell defect in these patients can be explained by the fact that IL-7 is not able to transduce its signal by the molecular defect of the common gamma (gamma c) chain and that IL-7 is indispensable for T-cell development.

摘要

当在体外接种到严重联合免疫缺陷(SCID)小鼠的分离胎儿胸腺叶中,随后进行胎儿胸腺器官培养(FTOC)时,高度纯化的人CD34 +胎儿肝干细胞可分化为成熟T细胞。在此,这种嵌合人 - 小鼠FTOC被用于研究白细胞介素-7(IL-7)和IL-7受体α链(IL-7Rα)在早期人类T细胞发育中的作用。我们报告称,添加可中和人和小鼠IL-7的单克隆抗体(MoAb)M25,或仅识别并阻断人IL-7R高亲和力α链的MoAb M21,都会导致人胸腺细胞数量大幅减少。对淋巴细胞亚群的分析表明,从CD34 +前体细胞向CD4 + CD3 - CD1 +祖细胞,随后向CD4 + CD8 +胸腺细胞成熟的细胞数量大幅减少。我们的结果揭示了IL-7在早期人类胸腺细胞发育中的关键作用,并可能解释了X连锁重症联合免疫缺陷患者中T细胞缺失或水平极低的现象。这些患者的分子缺陷已被证明是IL-2Rγ链中的突变。尽管该γ链不仅存在于IL-2R中,还构成其他细胞因子受体(包括IL-4、IL-7、IL-9、IL-13和IL-15)的重要组成部分,但这些患者的T细胞缺陷可以通过以下事实来解释:IL-7无法通过常见γ(γc)链的分子缺陷转导其信号,且IL-7对T细胞发育不可或缺。

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1
Interleukin-7 is a critical growth factor in early human T-cell development.白细胞介素-7是人类早期T细胞发育中的关键生长因子。
Blood. 1996 Dec 1;88(11):4239-45.
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Human CD34+ fetal liver stem cells differentiate to T cells in a mouse thymic microenvironment.人类CD34+胎肝干细胞在小鼠胸腺微环境中分化为T细胞。
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Precursors of CD3+CD4+CD8+ cells in the human thymus are defined by expression of CD34. Delineation of early events in human thymic development.人类胸腺中CD3+CD4+CD8+细胞的前体由CD34的表达来定义。人类胸腺发育早期事件的描述。
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The common gamma-chain of cytokine receptors regulates intrathymic T cell development at multiple stages.细胞因子受体的共同γ链在多个阶段调节胸腺内T细胞的发育。
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Cytokine dependence of V gamma 3 thymocytes: mature but not immature V gamma 3 cells require endogenous IL-2 and IL-7 to survive--evidence for cytokine redundancy.
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Stromal cell-derived factor 1/CXCR4 signaling is critical for early human T-cell development.基质细胞衍生因子1/CXCR4信号通路对人类T细胞早期发育至关重要。
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Implication of the common gamma chain of the IL-7 receptor in intrathymic development of pro-T cells.白细胞介素-7受体的共同γ链在胸腺内前T细胞发育中的作用
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Generation of T cells from adult human hematopoietic stem cells and progenitors in a fetal thymic organ culture system: stimulation by tumor necrosis factor-alpha.在胎儿胸腺器官培养系统中由成人造血干细胞和祖细胞生成T细胞:肿瘤坏死因子-α的刺激作用
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Differential effects of interleukin-15 and interleukin-2 on differentiation of bipotential T/natural killer progenitor cells.白细胞介素-15和白细胞介素-2对双潜能T/自然杀伤祖细胞分化的不同作用。
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