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人树突状细胞。从外周血中富集与鉴定。

Human dendritic cells. Enrichment and characterization from peripheral blood.

作者信息

Van Voorhis W C, Hair L S, Steinman R M, Kaplan G

出版信息

J Exp Med. 1982 Apr 1;155(4):1172-87. doi: 10.1084/jem.155.4.1172.

Abstract

Previous studies demonstrated that lymphoid tissues of mice and rats contain small numbers (less than 1 percent of nucleated cells) of dendritic cells (DC) with special cytologic, surface, and functional properties. We show here that similar DC represent 0.1-0.5 percent of human peripheral blood mononuclear cells. DC can be enriched to 20-60 percent purity by a multistep procedure analogous to that used in mice. Adherent peripheral blood mononuclear cells are cultured overnight, and the released cells are depleted of monocytes and B cells by readherence to plastic, rosetting with erythrocytes coated with anti-human IgG, and centrifugation in dense albumin columns. Enriched DC have similar cytologic features to rodent DC by light and electron microscopy. DC express HLA, and HLA-DR and the leukocyte-common antigens. They lack phagocytic capacity, receptors for antibody-coated and neuraminidase-treated erythrocytes, surface and intracellular Ig, esterase, peroxidase, and azurophilic granules. DC do not react with several monoclonal antibodies directed to phagocytes (OKM 1, "mac-1," 63D3, and 61D3) and T cells (OKT 3, 6, 8). Unlike the mouse, human DC express complement receptors. When maintained in culture for 4 d, human DC did not give rise to either B cells or monocytes. Therefore, DC identified by cytologic criteria are distinct from other leukocytes. Enriched populations of DC have been compared to fractions enriched in monocytes, B cells, and T cells in three functional assays: stimulation of the primary allogeneic mixed leukocyte reaction, stimulation of the primary syngeneic MLR, and accessory function for the proliferation of periodate- modified T cells. In each case, the DC fraction was 10-fold or more active than other cell fractions. We conclude that DC circulate in man, and represent the principal cell type required for the initiation of several immune responses.

摘要

以往的研究表明,小鼠和大鼠的淋巴组织含有少量(占有核细胞的不到1%)具有特殊细胞学、表面和功能特性的树突状细胞(DC)。我们在此表明,类似的DC占人类外周血单个核细胞的0.1 - 0.5%。通过类似于用于小鼠的多步骤程序,DC可富集至纯度为20 - 60%。贴壁的外周血单个核细胞培养过夜,通过再次贴壁于塑料培养皿、与包被抗人IgG的红细胞进行玫瑰花结形成以及在浓白蛋白柱中离心,去除释放细胞中的单核细胞和B细胞。通过光镜和电镜观察,富集的DC具有与啮齿动物DC相似的细胞学特征。DC表达HLA、HLA - DR以及白细胞共同抗原。它们缺乏吞噬能力、针对抗体包被和神经氨酸酶处理红细胞的受体、表面和细胞内Ig、酯酶、过氧化物酶以及嗜天青颗粒。DC不与几种针对吞噬细胞(OKM 1、“mac - 1”、63D3和61D3)和T细胞(OKT 3、6、8)的单克隆抗体发生反应。与小鼠不同,人类DC表达补体受体。当在培养中维持4天时,人类DC既不产生B细胞也不产生单核细胞。因此,根据细胞学标准鉴定的DC与其他白细胞不同。在三种功能测定中,已将富集的DC群体与富集单核细胞、B细胞和T细胞的组分进行了比较:刺激原发性同种异体混合淋巴细胞反应、刺激原发性同基因MLR以及对高碘酸盐修饰T细胞增殖的辅助功能。在每种情况下,DC组分的活性比其他细胞组分高10倍或更多。我们得出结论,DC在人体内循环,并且代表启动几种免疫反应所需的主要细胞类型。

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