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人单核细胞的体外分化。在玻璃或胶原蛋白上培养诱导的单核细胞表型差异。

In vitro differentiation of human monocytes. Differences in monocyte phenotypes induced by cultivation on glass or on collagen.

作者信息

Kaplan G, Gaudernack G

出版信息

J Exp Med. 1982 Oct 1;156(4):1101-14. doi: 10.1084/jem.156.4.1101.

Abstract

We demonstrated that the in vitro differentiation of human peripheral blood monocytes to macrophages is dependent on the environment and conditions of monocyte culture. Cultivation of monocytes on glass or microexudate-coated glass gave rise to cells resembling foreign body granuloma macrophages. After an initial rise in Fc receptor- and C3 receptor-mediated phagocytosis, a progressive loss of Fc receptor expression and C3-mediated ingestion were observed. The monocyte surface antigens recognized by the anti-human monocyte monoclonal antibodies 1D5 and 63D3 were lost from the surface of the majority of cells cultured on glass and microexudates. A subpopulation of Fc receptor-positive cells that were 1D5 and 63D3 positive was retained in fully differentiated cell populations. In comparison, monocytes cultivated on collagen matrices gave rise to highly phagocytic cells resembling human resident tissue macrophages. Both Fc- and C3-mediated phagocytosis were enhanced and remained so during the entire length of culture. The surface antigens recognized by the 1D5 antibody, expressed on all freshly seeded monocytes, was maintained on the macrophages. The antigen recognized by the 63D3 antibody was not expressed on mature cells. The present evidence would indicate that variations in expression of phagocytic receptors and the surface antigens 1D5 and 63D3 can be ascribed to the stage of development of the macrophage or its stage of activation, rather than to independent subsets of mononuclear phagocytes.

摘要

我们证明,人外周血单核细胞向巨噬细胞的体外分化取决于单核细胞培养的环境和条件。在玻璃或微渗出物包被的玻璃上培养单核细胞会产生类似于异物肉芽肿巨噬细胞的细胞。在Fc受体和C3受体介导的吞噬作用最初升高后,观察到Fc受体表达逐渐丧失以及C3介导的摄取作用减弱。抗人单核细胞单克隆抗体1D5和63D3识别的单核细胞表面抗原在玻璃和微渗出物上培养的大多数细胞表面消失。在完全分化的细胞群体中保留了一个Fc受体阳性且1D5和63D3阳性的亚群。相比之下,在胶原蛋白基质上培养的单核细胞产生了高度吞噬性的细胞,类似于人类驻留组织巨噬细胞。Fc和C3介导的吞噬作用均增强,并且在整个培养过程中一直保持增强。1D5抗体识别的表面抗原在所有新接种的单核细胞上均有表达,并在巨噬细胞上得以维持。63D3抗体识别的抗原在成熟细胞上不表达。目前的证据表明,吞噬受体以及表面抗原1D5和63D3表达的变化可归因于巨噬细胞的发育阶段或其激活阶段,而不是单核吞噬细胞的独立亚群。

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