首页> 美国卫生研究院文献>Journal of the Boston Society of Medical Sciences >Fc-receptor-bearing macrophages isolated from hypersensitivity and foreign-body granulomas. Delineation of macrophage dynamics fc receptor density/avidity and specificity.
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Fc-receptor-bearing macrophages isolated from hypersensitivity and foreign-body granulomas. Delineation of macrophage dynamics fc receptor density/avidity and specificity.

机译:从超敏反应和异物肉芽肿中分离出来的带有Fc受体的巨噬细胞。巨噬细胞动力学fc受体密度/亲和力和特异性的描绘。

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摘要

Foreign-body and delayed hypersensitivity granulomas were induced in mice; and the dynamics of macrophages isolated from dispersed, 1--4-week-old lesions was delineated. The size and histologic complexity of the lesions increased as shown: adjuvant greater than schistosome egg greater than methylated bovine serum albumin greater than bead. Esterase staining, spreading on glass, and the percentage of Fc-receptor--bearing macrophages present in the various granulomas reflected the same gradient. The Fc receptors were examined by rosetting with rabbit-antibody--SRBC complex (EA). Whereas more than 90% of the population of macrophages of the dermal adjuvant granuloma contained undiminished numbers of receptor-bearing macrophages throughout the 4 weeks, the percentage of macrophages that displayed receptors in pulmonary foreign-body (40%) and delayed hypersensitivity granulomas (70%) peaked at 1 week and subsequently declined. The EA rosetting of the foreign-body and delayed hypersensitivity granuloma macrophages was strongly inhibited by monomeric IgG2a-specific and weakly by aggregated IgG2b-specific mouse myeloma proteins. Also, macrophages of the delayed hypersensitivity granulomas rosetted in higher percentages with SRBCs coupled with monomeric IgC2a than with those coupled with aggregated IgG2b myeloma proteins. Macrophages of the foreign-body lesion did not react with aggregated IgG2b--SRBC. Rosetting with monomeric IgG2a--SRBC or aggregated IgG2b--SRBC could not be cross-inhibited by the myeloma proteins. Both the monomeric IgG2a--SRBC and aggregated IgG2b--SRBC complexes were readily phagocytized. Trypsin treatment of the macrophages inhibited rosetting with EA or myeloma-protein--coupled SRBCs. The display of Fc receptors on the granuloma macrophages seems to be related to the etiology of the lesion and the intensity and duration of the inflammatory reaction.
机译:在小鼠中诱发异物和迟发型超敏性肉芽肿;描绘了从分散的1-4周龄病变中分离出来的巨噬细胞的动力学。如图所示,病变的大小和组织学复杂性增加:佐剂大于血吸虫卵,大于甲基化牛血清白蛋白,大于珠。酯酶染色,铺展在玻璃上以及各种肉芽肿中带有Fc受体的巨噬细胞百分比反映了相同的梯度。通过用兔抗体-SRBC复合物(EA)玫瑰花结检查Fc受体。在整个4周中,超过90%的皮肤佐剂性肉芽肿巨噬细胞中携带受体的巨噬细胞数量没有减少,而在肺异物中表现出受体的巨噬细胞的百分比(40%)和迟发型超敏性肉芽肿(70%) %)在第1周达到顶峰,随后下降。异体抗体和迟发型超敏性肉芽肿巨噬细胞的EA花结被单体IgG2a特异性强烈抑制,而被IgG2b特异性聚集的小鼠骨髓瘤蛋白则弱抑制。而且,与结合单体IgC2a的SRBCs相比,延迟超敏性肉芽肿的巨噬细胞与那些与聚集的IgG2b骨髓瘤蛋白结合的巨噬细胞上升的百分比更高。异物病变的巨噬细胞不与聚集的IgG2b-SRBC反应。用单体IgG2a-SRBC或聚集的IgG2b-SRBC进行的玫瑰花结不能被骨髓瘤蛋白交叉抑制。单体IgG2a-SRBC和聚集的IgG2b-SRBC复合物都容易被吞噬。胰蛋白酶处理巨噬细胞可抑制EA或骨髓瘤蛋白偶联的SRBC的玫瑰花结。肉芽肿巨噬细胞上Fc受体的出现似乎与病变的病因以及炎症反应的强度和持续时间有关。

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