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胸腺中的 T 细胞分化。

T cell differentiation in the thymus.

机构信息

Department of Anatomy and Biochemistry, University of Genova, Genova, Italy.

出版信息

Cytotechnology. 1991 Feb;5(Suppl 1):113-6. doi: 10.1007/BF00736825.

Abstract

T lymphocytes arise in the thymus and seed to peripheral lymphoid organs as fully functional cells at the time of exit. In humans, the thymus begins to function very early in ontogeny and releases large numbers of T cells before the time of birth. However, the vast majority of developing thymocytes (>95%) die within the thymus as a result of stringent selection processes. Positive selection imposes self-MHC-restriction on thymocytes and dictates the MHC-restricted repertoire of post-thymic T cells. Negative selection results in deletion of autoreactive cells. Both types of selection depend on cell to cell contracts and on the presence of appropriate growth factors which are still largely undetermined. Cell to cell contacts occur between developing thymocytes and cells of the thymic microenvironment (accessory cells), and are mediated by several receptor/ligand interactions which subserve the function of establishing and stabilizing these contacts. Besides MHC-TCR interactions, adhesion molecules are important for thymocyte maturation, selection and activation, and for the export and peripheral homing of mature T cells produced in the thymus. Here we describe a novel integrin involved in thymocyte-thymic epithelial cell interactions.

摘要

T 淋巴细胞在胸腺中产生,并在离开胸腺时作为成熟的功能性细胞播种到外周淋巴器官中。在人类中,胸腺在胚胎发育早期就开始发挥作用,并在出生前释放大量 T 细胞。然而,绝大多数发育中的胸腺细胞(>95%)由于严格的选择过程而在胸腺内死亡。阳性选择对胸腺细胞施加自身 MHC 限制,并决定了胸腺后 T 细胞的 MHC 限制 repertoire。阴性选择导致自身反应性细胞的删除。这两种选择都依赖于细胞间的接触以及适当的生长因子的存在,而这些生长因子在很大程度上仍未确定。细胞间接触发生在发育中的胸腺细胞和胸腺微环境(辅助细胞)之间,由几种受体/配体相互作用介导,这些相互作用有助于建立和稳定这些接触。除了 MHC-TCR 相互作用外,粘附分子对于胸腺细胞的成熟、选择和激活,以及在胸腺中产生的成熟 T 细胞的输出和外周归巢也很重要。在这里,我们描述了一种参与胸腺细胞-胸腺上皮细胞相互作用的新型整合素。

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