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原胸腺细胞亚群调控胸腺皮质诱导中的发育控制点。

Developmental control point in induction of thymic cortex regulated by a subpopulation of prothymocytes.

作者信息

Holländer G A, Wang B, Nichogiannopoulou A, Platenburg P P, van Ewijk W, Burakoff S J, Gutierrez-Ramos J C, Terhorst C

机构信息

Division of Pediatric Oncology, Dana-Farber Cancer Institute, Harvard Medical School, Boston, Massachusetts 02115.

出版信息

Nature. 1995 Jan 26;373(6512):350-3. doi: 10.1038/373350a0.

DOI:10.1038/373350a0
PMID:7830770
Abstract

T lymphocytes of the alpha/beta T-cell receptor (TCR) lineage mature in the thymus, where they undergo a series of differentiation, expansion and selection events. For normal T-cell ontogeny to occur, thymocytes must interact physically with cortical and medullary thymic stroma cells. In parallel, interactions of the thymic stromal cells with TCR-positive thymocytes are necessary for the development of the thymic medulla. Comparable requirements for the differentiation of the cortex have not been defined, however. Here we analyse mutant mouse strains to assess the function of early prothymocytes in the induction of the thymic cortex. We find that animals with a developmental block at the earliest stage of T-lineage commitment lack a functional thymic cortex. This abnormality could be corrected in fetal but not adult animals by transplantation of either fetal or adult wild-type haematopoietic stem cells. Thus a developmentally restricted interaction of fetal stromal cells with early prothymocytes is required for the induction of a cortical microenvironment. In addition, a normal thymic architecture is necessary for sustained T-cell ontogeny.

摘要

α/βT细胞受体(TCR)谱系的T淋巴细胞在胸腺中成熟,它们在胸腺经历一系列分化、扩增和选择事件。为了使正常的T细胞个体发育得以发生,胸腺细胞必须与皮质和髓质胸腺基质细胞进行物理相互作用。同时,胸腺基质细胞与TCR阳性胸腺细胞的相互作用对于胸腺髓质的发育是必需的。然而,对于皮质分化的类似要求尚未明确。在这里,我们分析突变小鼠品系以评估早期原胸腺细胞在诱导胸腺皮质中的功能。我们发现,在T细胞谱系定向的最早阶段出现发育阻滞的动物缺乏功能性胸腺皮质。通过移植胎儿或成年野生型造血干细胞,这种异常在胎儿而非成年动物中可以得到纠正。因此,胎儿基质细胞与早期原胸腺细胞之间发育受限的相互作用是诱导皮质微环境所必需的。此外,正常的胸腺结构对于持续的T细胞个体发育是必要的。

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