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通过一种皮质胸腺上皮细胞系对II类限制性TCR转基因胸腺细胞进行体外阳性选择和无能诱导。

In vitro positive selection and anergy induction of class II-restricted TCR transgenic thymocytes by a cortical thymic epithelial cell line.

作者信息

Nelson A J, Clegg C H, Farr A G

机构信息

Department of Biological Structure, University of Washington, Seattle, USA.

出版信息

Int Immunol. 1998 Sep;10(9):1335-46. doi: 10.1093/intimm/10.9.1335.

Abstract

Thymic epithelial cell lines isolated from hyperplastic thymi of transgenic mice over-expressing human papilloma viral oncogenes E6 and E7 constitutively displayed a phenotype consistent with a cortical origin. Exposure to IFN-gamma induced class II MHC and ICAM-1 expression, and up-regulated expression of VCAM-1 and class I MHC molecules. CD40 expression was maximally induced by a combination of IFN-gamma and IL-1, with lower levels of induction observed with a mixture of IFN-gamma and tumor necrosis factor (TNF)-alpha or TNF-alpha alone. B7-1 or B7-2 was not expressed constitutively or in response to cytokines. These stromal cells supported the development of CD4 single-positive (SP) cells in reaggregate co-cultures with CD4+ CD8+ thymocytes from TCR transgenic mice, but did not stimulate class II MHC-restricted, moth cytochrome c (MCC)-reactive T cells in vitro. The behavior of the culture system was consistent with positive selection, i.e. increased numbers of CD4 SP cells, gain of antigen responsiveness, and requirement for epithelial class II MHC products. Some variants of these stromal cell lines required exogenous MCC peptide in the reaggregation cultures (RC) for positive selection to occur. While a low concentration of MCC peptide (0.01-0.1 microM) significantly enhanced the accumulation of CD4 SP cells, higher concentrations of peptide (1-10 microM) resulted in recovery of predominantly CD4- CD8- and CD4(low) CD8- cells. Thymocytes recovered from RC containing low, but not high concentrations of peptide responded to MCC peptide in secondary cultures with splenic antigen-presenting cells.

摘要

从过度表达人乳头瘤病毒致癌基因E6和E7的转基因小鼠增生胸腺中分离出的胸腺上皮细胞系,其表型始终与皮质来源一致。暴露于γ干扰素可诱导II类主要组织相容性复合体(MHC)和细胞间黏附分子-1(ICAM-1)的表达,并上调血管细胞黏附分子-1(VCAM-1)和I类MHC分子的表达。CD40的表达在γ干扰素和白细胞介素-1共同作用下诱导程度最大,而γ干扰素与肿瘤坏死因子(TNF)-α混合或单独使用TNF-α时,诱导水平较低。B7-1或B7-2在正常情况下不表达,也不响应细胞因子。这些基质细胞在与T细胞受体转基因小鼠的CD4+CD8+胸腺细胞进行重聚集共培养时,支持CD4单阳性(SP)细胞的发育,但在体外不刺激II类MHC限制的、蛾细胞色素c(MCC)反应性T细胞。培养系统的行为与阳性选择一致,即CD4 SP细胞数量增加、获得抗原反应性以及对上皮II类MHC产物的需求。这些基质细胞系的一些变体在重聚集培养(RC)中需要外源性MCC肽才能发生阳性选择。虽然低浓度的MCC肽(0.01 - 0.1微摩尔)显著增强了CD4 SP细胞的积累,但较高浓度的肽(1 - 10微摩尔)导致主要恢复的是CD4-CD8-和CD4(低)CD8-细胞。从含有低浓度而非高浓度肽的RC中回收的胸腺细胞,在与脾抗原呈递细胞进行的二次培养中对MCC肽有反应。

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