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Human blood contains two subsets of dendritic cells one immunologically mature and the other immature.

机译:人体血液包含树突状细胞的两个子集一个子集免疫成熟另一个未成熟。

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摘要

Two subsets of dendritic cells, differing in T-cell stimulatory function, have been purified directly from human blood. Both subsets are positive for major histocompatibility complex (MHC) class II expression and negative for lineage-specific antigens (e.g. CD3, CD14, CD16, CD19 negative), but are separated by exploiting differences in expression of the beta 2-integrin, CD11c. The CD11c-negative subset is functionally immature, requiring monocyte-derived cytokines to develop into typical dendritic cells. The CD11c-positive subset has potent T-cell stimulating activity and expresses the activation antigen CD45RO, unlike its immature counterpart. However, these mature cells only develop typical dendritic morphology and high levels of MHC proteins and adhesins after a period of culture independent of exogenous cytokines. Although the freshly isolated mature dendritic cells resemble monocytes in cytospin preparations, the former lack CD14 and have a much stronger primary T-cell stimulatory capacity. We hypothesize that the CD11c-negative immature cells are marrow-derived precursors to tissue dendritic cells, such as epidermal Langerhans' cells, while the CD11c-positive cells are derived from tissues where they have been activated by antigen, and are en route to the spleen or lymph nodes to stimulate T-cell responses there.
机译:已经从人血中直接纯化了两个亚群的树突状细胞,它们的T细胞刺激功能不同。这两个亚组的主要组织相容性复合物(MHC)II类表达均为阳性,而谱系特异性抗原(例如CD3,CD14,CD16,CD19阴性)均为阴性,但通过利用β2-整联蛋白CD11c表达差异将它们分开。 CD11c阴性亚群功能不成熟,需要单核细胞衍生的细胞因子才能发育成典型的树突状细胞。 CD11c阳性子集具有强大的T细胞刺激活性,并表达活化抗原CD45RO,这与其未成熟的对应物不同。然而,这些成熟的细胞经过一段独立于外源细胞因子的培养后,仅会发展出典型的树突形态,并产生高水平的MHC蛋白和粘附素。尽管新鲜分离的成熟树突状细胞类似于cytospin制剂中的单核细胞,但前者缺乏CD14,并且具有更强的初级T细胞刺激能力。我们假设CD11c阴性的未成熟细胞是组织树突状细胞(如表皮朗格汉斯细胞)的骨髓来源的前体,而CD11c阳性的细胞则来自被抗原激活的组织,并且正途经脾或淋巴结刺激那里的T细胞反应。

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