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从人血液中新鲜分离的树突状细胞表达CD4,并在单核细胞条件培养基中培养后成熟为典型的免疫刺激性树突状细胞。

Dendritic cells freshly isolated from human blood express CD4 and mature into typical immunostimulatory dendritic cells after culture in monocyte-conditioned medium.

作者信息

O'Doherty U, Steinman R M, Peng M, Cameron P U, Gezelter S, Kopeloff I, Swiggard W J, Pope M, Bhardwaj N

机构信息

Laboratory of Cellular Physiology and Immunology, Rockefeller University, New York, New York 10021.

出版信息

J Exp Med. 1993 Sep 1;178(3):1067-76. doi: 10.1084/jem.178.3.1067.

Abstract

A procedure has been developed to isolate dendritic cells to a high degree of purity from fresh blood. Prior enrichment methods have relied upon an initial 1-2-d culture period. Purified fresh isolates lack the characteristic morphology, phenotype, and immunostimulatory function of dendritic cells. The purified cells have the appearance of medium sized lymphocytes and express substantial levels of CD4, but lack the T cell molecules CD3, CD8, and T cell receptor. When placed in culture, the cells mature in a manner resembling the previously described, cytokine-dependent maturation of epidermal dendritic cells (Langerhans cells). The cells enlarge and exhibit many cell processes, express much higher levels of major histocompatibility complex class II and a panel of accessory molecules for T cell activation, and become potent stimulators of the mixed leukocyte reaction. Among the many changes during this maturation process are a fall in CD4 and the appearance of high levels of B7/BB1, the costimulator for enhanced interleukin 2 production in T cells. These changes are not associated with cell proliferation, but are dependent upon the addition of monocyte-conditioned medium. We suggest that the freshly isolated CD4-positive blood dendritic cells are recent migrants from the bone marrow, and that subsequent maturation of the lineage occurs in tissues in situ upon appropriate exposure to cytokines.

摘要

已开发出一种从新鲜血液中高度纯化分离树突状细胞的方法。先前的富集方法依赖于最初1 - 2天的培养期。纯化的新鲜分离物缺乏树突状细胞的特征形态、表型和免疫刺激功能。纯化后的细胞呈中等大小淋巴细胞外观,表达大量CD4,但缺乏T细胞分子CD3、CD8和T细胞受体。置于培养中时,这些细胞以类似于先前描述的表皮树突状细胞(朗格汉斯细胞)细胞因子依赖性成熟的方式成熟。细胞体积增大并呈现许多细胞突起,表达更高水平的主要组织相容性复合体II类分子和一组用于T细胞激活的辅助分子,并成为混合淋巴细胞反应的强效刺激剂。在这个成熟过程中的许多变化包括CD4水平下降以及高水平B7/BB1的出现,B7/BB1是增强T细胞中白细胞介素2产生的共刺激分子。这些变化与细胞增殖无关,而是依赖于添加单核细胞条件培养基。我们认为,新鲜分离的CD4阳性血液树突状细胞是最近从骨髓迁移而来的,并且该细胞系随后在组织原位经适当暴露于细胞因子后发生成熟。

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