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The kinetics of T cell antigen receptor expression by subgroups of CD4+8+ thymocytes: delineation of CD4+8+3(2+) thymocytes as post-selection intermediates leading to mature T cells.CD4+8+胸腺细胞亚群T细胞抗原受体表达的动力学:将CD4+8+3(2+)胸腺细胞描绘为通向成熟T细胞的选择后中间体。
J Exp Med. 1991 Feb 1;173(2):323-32. doi: 10.1084/jem.173.2.323.
2
Different subpopulations of developing thymocytes are associated with adherent (macrophage) or nonadherent (dendritic) thymic rosettes.发育中的胸腺细胞的不同亚群与贴壁(巨噬细胞)或非贴壁(树突状)胸腺花环相关。
Dev Immunol. 1991;1(3):225-35. doi: 10.1155/1991/49025.
3
Subpopulations of mature murine thymocytes: properties of CD4-CD8+ and CD4+CD8- thymocytes lacking the heat-stable antigen.成熟小鼠胸腺细胞的亚群:缺乏热稳定抗原的CD4-CD8+和CD4+CD8-胸腺细胞的特性
Cell Immunol. 1988 Dec;117(2):312-26. doi: 10.1016/0008-8749(88)90121-9.
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Fc gamma RII/III and CD2 expression mark distinct subpopulations of immature CD4-CD8- murine thymocytes: in vivo developmental kinetics and T cell receptor beta chain rearrangement status.FcγRII/III和CD2表达标记未成熟CD4-CD8-小鼠胸腺细胞的不同亚群:体内发育动力学和T细胞受体β链重排状态。
J Exp Med. 1993 Apr 1;177(4):1079-92. doi: 10.1084/jem.177.4.1079.
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Kinetics of mature T-cell development in the thymus.胸腺中成熟T细胞发育的动力学
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In vivo modulation of the distribution of thymocyte subsets: effects of estrogen on the expression of different T cell receptor V beta gene families in CD4-, CD8- thymocytes.体内胸腺细胞亚群分布的调节:雌激素对CD4 -、CD8 -胸腺细胞中不同T细胞受体Vβ基因家族表达的影响。
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Delineation of chicken thymocytes by CD3-TCR complex, CD4 and CD8 antigen expression reveals phylogenically conserved and novel thymocyte subsets.通过CD3-TCR复合体、CD4和CD8抗原表达对鸡胸腺细胞进行描绘,揭示了系统发育上保守的和新的胸腺细胞亚群。
Int Immunol. 1992 Oct;4(10):1175-82. doi: 10.1093/intimm/4.10.1175.
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Programmed differentiation of murine thymocytes during fetal thymus organ culture.胎儿胸腺器官培养过程中小鼠胸腺细胞的程序性分化。
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Alpha/beta heterodimeric T-cell receptor expression early in thymocyte differentiation.α/β异二聚体T细胞受体在胸腺细胞分化早期的表达。
J Mol Cell Immunol. 1988;3(6):347-62.
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Evidence for susceptibility of intrathymic T-cell precursors and their progeny carrying T-cell antigen receptor phenotypes TCR alpha beta + and TCR gamma delta + to human immunodeficiency virus infection: a mechanism for CD4+ (T4) lymphocyte depletion.胸腺内携带T细胞抗原受体表型TCRαβ+和TCRγδ+的T细胞前体及其子代对人类免疫缺陷病毒感染易感性的证据:一种CD4+(T4)淋巴细胞耗竭的机制。
Proc Natl Acad Sci U S A. 1990 Oct;87(19):7727-31. doi: 10.1073/pnas.87.19.7727.

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Immune tolerance and the prevention of autoimmune diseases essentially depend on thymic tissue homeostasis.免疫耐受和自身免疫性疾病的预防从根本上取决于胸腺组织的稳态。
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Agonist-selected T cell development requires strong T cell receptor signaling and store-operated calcium entry.激动剂选择的 T 细胞发育需要强大的 T 细胞受体信号和储存操作的钙内流。
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8
Role of gonadal hormones in programming developmental changes in thymopoietic efficiency and sexual diergism in thymopoiesis.性腺激素在编程胸腺生成效率的发育变化和胸腺生成中的性二态性中的作用。
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Gads-deficient thymocytes are blocked at the transitional single positive CD4+ stage.缺乏Gads的胸腺细胞在过渡性单阳性CD4+阶段受阻。
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Calcineurin sets the bandwidth for discrimination of signals during thymocyte development.钙调神经磷酸酶在胸腺细胞发育过程中设定了信号识别的带宽。
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Thymus cell migration. Quantitative aspects of cellular traffic from the thymus to the periphery in mice.胸腺细胞迁移。小鼠体内细胞从胸腺向外周迁移的定量研究。
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Acquisition of immune competence by a subset of human cortical thymocytes expressing mature T cell antigens.表达成熟T细胞抗原的人类皮质胸腺细胞亚群获得免疫能力。
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Characterization of the murine T cell surface molecule, designated L3T4, identified by monoclonal antibody GK1.5: similarity of L3T4 to the human Leu-3/T4 molecule.用单克隆抗体GK1.5鉴定的小鼠T细胞表面分子L3T4的特性:L3T4与人Leu-3/T4分子的相似性
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A T cell receptor V beta segment that imparts reactivity to a class II major histocompatibility complex product.一种赋予对II类主要组织相容性复合体产物反应性的T细胞受体Vβ区段。
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Positive selection of CD4+ thymocytes controlled by MHC class II gene products.由MHC II类基因产物控制的CD4+胸腺细胞的阳性选择。
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Selective expression of an antigen receptor on CD8-bearing T lymphocytes in transgenic mice.转基因小鼠中携带CD8的T淋巴细胞上抗原受体的选择性表达。
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CD4+8+胸腺细胞亚群T细胞抗原受体表达的动力学:将CD4+8+3(2+)胸腺细胞描绘为通向成熟T细胞的选择后中间体。

The kinetics of T cell antigen receptor expression by subgroups of CD4+8+ thymocytes: delineation of CD4+8+3(2+) thymocytes as post-selection intermediates leading to mature T cells.

作者信息

Shortman K, Vremec D, Egerton M

机构信息

Walter and Eliza Hall Institute of Medical Research, Melbourne, Victoria, Australia.

出版信息

J Exp Med. 1991 Feb 1;173(2):323-32. doi: 10.1084/jem.173.2.323.

DOI:10.1084/jem.173.2.323
PMID:1824855
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2118785/
Abstract

Cortical thymocytes from adult mice, separated on the basis of coexpression of CD4 and CD8 or of binding of high levels of peanut agglutinin (PNA), were subdivided according to the level of expression of the T cell receptor (TCR)-CD3 complex. The incidence of dividing cells in the resultant subpopulations was determined by DNA staining. Precursor-product relationships and the timing of TCR-CD3 acquisition were studied using continuous in vivo [3H]TdR labeling and radioautography. The extent of intrathymic selection for TCR specificity in the subpopulations was determined from the incidence of cells bearing V beta 6 or V beta 17a in different mouse strains. The majority of dividing CD4+8+ blast cells expressed extremely low levels of TCR-CD3, indicating that TCR expression and specificity selection generally occurred after division ceased. The [3H]TdR-labeling studies indicated that postdivision TCR expression was rapid, and that those nondividing cortical thymocytes which had not expressed significant levels of TCR by day 1, remained extremely low or negative for their entire 3.6-d lifespan. Small cortical thymocytes which expressed moderate levels of TCR-CD3, were predominantly an unselected population with a lifespan of 3.8 d. A small subgroup of CD4+8+ PNA+ cortical thymocytes expressing high levels of TCR-CD3 was identified as a nondividing intermediate between the small cortical thymocytes expressing moderate levels of TCR and mature medullary thymocytes. These intermediates showed a 1-d lag in [3H]TdR labeling, then a 3.4-d transit time. The cell flux through this intermediate subpopulation was approximately 10(6) cells/d, similar to the rate of turnover of mature thymocytes; thus, although only 3-4% of thymocytes progressed to this intermediate state, once reaching it most then progressed to full maturity. In accordance with this, the incidence of the V beta selection markers within the intermediate subpopulation indicated that both positive and negative selection had already occurred. Selection for TCR specificity in the systems studied appeared to take place among CD4+8+ thymocytes expressing intermediate levels of TCR.

摘要

根据CD4和CD8的共表达或高水平花生凝集素(PNA)的结合情况分离出的成年小鼠皮质胸腺细胞,再根据T细胞受体(TCR)-CD3复合物的表达水平进行细分。通过DNA染色确定所得亚群中分裂细胞的发生率。使用连续体内[3H]TdR标记和放射自显影研究前体-产物关系以及TCR-CD3获得的时间。根据不同小鼠品系中携带Vβ6或Vβ17a的细胞发生率,确定亚群中TCR特异性的胸腺内选择程度。大多数分裂的CD4+8+母细胞表达极低水平的TCR-CD3,这表明TCR表达和特异性选择通常在分裂停止后发生。[3H]TdR标记研究表明,分裂后TCR表达迅速,那些在第1天尚未表达显著水平TCR的非分裂皮质胸腺细胞,在其整个3.6天的寿命中仍保持极低水平或阴性。表达中等水平TCR-CD3的小皮质胸腺细胞主要是一个未被选择的群体,寿命为3.8天。一小部分表达高水平TCR-CD3的CD4+8+PNA+皮质胸腺细胞被鉴定为表达中等水平TCR的小皮质胸腺细胞和成熟髓质胸腺细胞之间的非分裂中间体。这些中间体在[3H]TdR标记中显示出1天的延迟,然后是3.4天的转运时间。通过这个中间亚群的细胞通量约为10^6个细胞/天,与成熟胸腺细胞的更新率相似;因此,尽管只有3-4%的胸腺细胞发展到这种中间状态,但一旦达到这种状态,大多数细胞随后会发展到完全成熟。据此,中间亚群中Vβ选择标记的发生率表明阳性和阴性选择都已经发生。在所研究的系统中,TCR特异性选择似乎发生在表达中等水平TCR的CD4+8+胸腺细胞中。