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单个干细胞可以重新定殖胚胎胸腺,产生表型不同的T细胞群体。

A single stem cell can recolonize an embryonic thymus, producing phenotypically distinct T-cell populations.

作者信息

Kingston R, Jenkinson E J, Owen J J

出版信息

Nature. 1985;317(6040):811-3. doi: 10.1038/317811a0.

DOI:10.1038/317811a0
PMID:3877245
Abstract

There is much interest in early T-cell development, particularly in relation to the diversification of the T-cell receptor repertoire and the elucidation of the lineage relationships between T-cell populations in the thymus and peripheral lymphoid organs. However, the requirements for the growth of the earliest thymic T-cell precursor in 13-14-day mouse embryo thymus in isolation from the thymic environment are unknown. Proliferation and maturation of such cells are not sustained either in the presence of monolayers of thymic stromal cells or by the addition of interleukin-2 (IL-2), despite the expression of receptors for this growth factor on a proportion of thymocytes displaying the immature Thy 1+ Lyt-2-L3T4- phenotype in the embryonic thymus. In contrast, when maintained within the intact thymic environment in organ cultures, 13-14-day thymic stem cells do show a pattern of surface marker and functional development similar to that seen in vivo, suggesting that short-range growth signals, perhaps necessitating direct contact with organized epithelial cells, are required. We have shown, by exploiting the selective toxicity of deoxyguanosine (dGuo) for early T cells, that this organ culture system can be manipulated to produce alymphoid lobes that can be recolonized from a source of precursors in a transfilter system. We now show that recolonization of alymphoid lobes can also be achieved by association with T-cell precursors in hanging drops, allowing recolonization by exposure to defined numbers of precursors, including a single micromanipulated stem cell. Analysis of T-cell marker expression in these cultures shows that a single thymic stem cell can produce progeny of distinct phenotypes, suggesting that these marker-defined populations are not derived from separate prethymic precursors, but arise within the thymus.

摘要

人们对早期T细胞发育非常感兴趣,特别是与T细胞受体库的多样化以及胸腺和外周淋巴器官中T细胞群体之间谱系关系的阐明有关。然而,13 - 14天小鼠胚胎胸腺中最早的胸腺T细胞前体在与胸腺环境隔离的情况下生长所需的条件尚不清楚。尽管在胚胎胸腺中一部分表现出未成熟Thy 1+ Lyt-2-L3T4-表型的胸腺细胞上表达了这种生长因子的受体,但在胸腺基质细胞单层存在的情况下或通过添加白细胞介素-2(IL-2),这些细胞的增殖和成熟都无法持续。相反,当在器官培养中维持在完整的胸腺环境中时,13 - 14天的胸腺干细胞确实表现出与体内相似的表面标志物和功能发育模式,这表明可能需要与有组织的上皮细胞直接接触的短程生长信号。我们已经通过利用脱氧鸟苷(dGuo)对早期T细胞的选择性毒性表明,这种器官培养系统可以被操纵以产生无淋巴细胞叶,这些叶可以在跨滤器系统中从前体来源重新定殖。我们现在表明,无淋巴细胞叶的重新定殖也可以通过与悬滴中的T细胞前体结合来实现,从而通过暴露于确定数量的前体,包括单个显微操作的干细胞来实现重新定殖。对这些培养物中T细胞标志物表达的分析表明,单个胸腺干细胞可以产生不同表型的后代,这表明这些由标志物定义的群体不是来自单独的胸腺前体,而是在胸腺内产生的。

相似文献

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A single stem cell can recolonize an embryonic thymus, producing phenotypically distinct T-cell populations.单个干细胞可以重新定殖胚胎胸腺,产生表型不同的T细胞群体。
Nature. 1985;317(6040):811-3. doi: 10.1038/317811a0.
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Day 11 mouse fetal thymus: phenotype and search for the point of commitment.第11天的小鼠胚胎胸腺:表型及寻找定向分化点
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Limited development capacity of the earliest embryonic murine thymus.最早的胚胎期小鼠胸腺的发育能力有限。
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Exogenous IL-7 promotes the growth of CD3-CD4-CD8-CD44+CD25+/- precursor cells and blocks the differentiation pathway of TCR-alpha beta cells in fetal thymus organ culture.外源性白细胞介素-7促进胎儿胸腺器官培养中CD3-CD4-CD8-CD44+CD25+/-前体细胞的生长,并阻断TCR-αβ细胞的分化途径。
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The phenotype of thymocytes derived from a single clonogenic precursor.源自单个克隆形成前体的胸腺细胞的表型。
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Differentiation of thymocytes in fetal organ culture: analysis of phenotypic changes accompanying the appearance of cytolytic and interleukin 2-producing cells.胎儿器官培养中胸腺细胞的分化:伴随溶细胞性细胞和白细胞介素2产生细胞出现的表型变化分析。
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Precursors of T cell growth factor producing cells in the thymus: ontogeny, frequency, and quantitative recovery in a subpopulation of phenotypically mature thymocytes defined by monoclonal antibody GK-1.5.胸腺中产生T细胞生长因子细胞的前体:由单克隆抗体GK-1.5定义的表型成熟胸腺细胞亚群中的个体发生、频率及定量回收
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T-cell differentiation in thymus organ cultures.胸腺器官培养中的T细胞分化。
Semin Immunol. 1990 Jan;2(1):51-8.

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