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主要组织相容性复合体结合肽在胎儿胸腺器官培养中诱导CD8 + T细胞的阳性选择。

Positive selection of CD8+ T cells induced by major histocompatibility complex binding peptides in fetal thymic organ culture.

作者信息

Hogquist K A, Gavin M A, Bevan M J

机构信息

Howard Hughes Medical Institute, Department of Immunology, University of Washington, Seattle 98195.

出版信息

J Exp Med. 1993 May 1;177(5):1469-73. doi: 10.1084/jem.177.5.1469.

Abstract

We have used an in vitro system to study the effects of major histocompatibility complex class I binding peptides on thymic development. Fetal thymus lobes from mice deficient in the class I light chain (beta 2 microglobulin or beta 2 M-/-) were cultured for 10 d in vitro, during which time T cell precursors develop into mature T cells. In these organ cultures, as in the adult or neonatal beta 2 M-/- thymus, CD8+ mature T cells did not develop, demonstrating that the mature T cells seen during early murine thymic development are the result of the positive selection process. To these cultures we added various class I binding peptides with or without a source of exogenous beta 2M. CD8+ T cells developed to various degrees only in the presence of beta 2M and peptides. Using peptide mixtures of differing complexity, we showed that the efficiency of this process is dependent more on peptide complexity than on peptide concentration. These data argue for a specific role for peptides in the process of positive selection. Furthermore, this culture system should be useful in identifying peptides that can promote positive selection of cells expressing a specific T cell receptor (TCR) in TCR transgenic mice.

摘要

我们利用体外系统研究主要组织相容性复合体I类结合肽对胸腺发育的影响。将I类轻链缺陷小鼠(β2微球蛋白缺陷或β2M -/-)的胎儿胸腺叶在体外培养10天,在此期间T细胞前体发育为成熟T细胞。在这些器官培养物中,如同在成年或新生β2M -/-胸腺中一样,CD8 +成熟T细胞未发育,这表明在小鼠胸腺早期发育过程中看到的成熟T细胞是阳性选择过程的结果。我们向这些培养物中添加了各种I类结合肽,有无外源性β2M来源。只有在存在β2M和肽的情况下,CD8 + T细胞才会不同程度地发育。使用不同复杂性的肽混合物,我们表明这一过程的效率更多地取决于肽的复杂性而非肽的浓度。这些数据表明肽在阳性选择过程中具有特定作用。此外,该培养系统应有助于鉴定能够促进TCR转基因小鼠中表达特定T细胞受体(TCR)的细胞进行阳性选择的肽。

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