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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Regulation of MHC Class I Transport in Human Dendritic Cells and the Dendritic-Like Cell Line KG-1.
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Regulation of MHC Class I Transport in Human Dendritic Cells and the Dendritic-Like Cell Line KG-1.

机译:人树突状细胞和类树突状细胞系KG-1中MHC I类转运的调控。

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摘要

Dendritic cells (DCs) progress through distinct maturational phases; immature DCs capture Ag while mature DCs are optimized for Ag presentation. Proper control of immunity requires regulated compartmentalization of MHC class II molecules. We report that DCs also regulate MHC class I trafficking throughout maturation. Although mature human DCs express high levels of surface MHC class I, immature DCs exhibit lower surface levels while retaining MHC class I-peptide complexes in the Golgi. A cell line, KG-1, behaves similarly. We confirm the similarity of KG-1 to DCs by demonstrating its capacity to present exogenous Ags in an MHC class I-restricted fashion to CD8(+) T cell hybridomas, a phenomenon called cross-presentation. Biochemical characterization of MHC class I trafficking throughout maturation showed that, in early KG-1 dendritic-like cells, surface arrival of MHC class I-peptide complexes is delayed by their retention in the Golgi. In mature dendritic-like cells, these complexes relocate to the surface and their stability increases, concomitant with up-regulation of costimulatory molecules. Maturation induces qualitative changes in the MHC class I-associated peptide repertoire demonstrated by increased thermostability. The differential processing of MHC class I throughout maturation may prevent premature immune activation while promoting T cell responses in lymph nodes to Ags acquired at sites of inflammation.
机译:树突状细胞(DC)经历了不同的成熟阶段。未成熟的DC捕获Ag,而成熟的DC已针对Ag展示进行了优化。正确控制免疫力需要调节MHC II类分子的区室化。我们报告说,DC在整个成熟过程中也对MHC I类交易进行监管。尽管成熟的人DC表现出高水平的I类表面MHC,但未成熟的DC表现出较低的表面水平,同时在高尔基体中保留了MHC I类-肽复合物。 KG-1细胞系的行为类似。我们通过证明其以MHC I类限制性方式向CD8(+)T细胞杂交瘤呈递外源Ags来证实KG-1与DC的相似性,这种现象称为交叉展示。在整个成熟过程中,MHC I类运输的生化特征表明,在早期KG-1树突状细胞中,MHC I类肽复合物的表面到达由于其在高尔基体中的滞留而延迟。在成熟的树突状细胞中,这些复合物重新定位到表面,并且其稳定性增加,同时伴随共刺激分子的上调。成熟引起了MHC I类相关肽库的定性变化,这由增加的热稳定性证明。在整个成熟过程中,MHC I类的差异加工可能会阻止免疫系统过早活化,同时促进淋巴结中的T细胞对炎症部位获得的Ag的反应。

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