Kodelja V, Goerdt S
Hautklinik, Universitätsklinikum Benjamin Franklin, Freie Universität Berlin, Germany.
Exp Dermatol. 1994 Dec;3(6):257-68. doi: 10.1111/j.1600-0625.1994.tb00287.x.
Macrophages play important roles in immunity and inflammation, and in allergic, granulomatous and neoplastic diseases. Here, we present the indepth results of an ongoing study of macrophage differentiation pathways in cutaneous macrophage disorders and in vitro. Up to now, a total of 40 cases of cutaneous macrophage disorders (histiocytoses and granulomas) and related diseases were examined using a panel of monoclonal and polyclonal antibodies to macrophage differentiation antigens (mAb MS-1, mAb alpha CD1a, mAb alpha CD34, mAb RM 3/1, mAb alpha CD11c, mAb alpha CD36, mAb MAC 387, mAb 27E10, polyclonal antibodies alpha MRP-8 and -14, mAb alpha CD68, mAb 25F9, mAb DRC1-R4/23, and mAb 1F10). Of these, MS-1 high molecular weight protein, synthesized by non-continuous sinusoidal endothelial cells and highly dendritic perivascular macrophages in normal human organs, is the most specific macrophage differentiation marker. MS-1 high molecular weight protein is selectively expressed by cutaneous non-Langerhans cell histocytoses, and proves to be a valuable diagnostic tool for these diseases. MS-1 high molecular weight protein is not found in Langerhans cell histiocytosis cells, epithelioid cells in sarcoidosis, and palisading histiocytes in granuloma annulare. MS-1+ macrophages may be found intermingled in cellular type dermatofibroma and in foreign body granulomas; they differ from MS-1+ non-Langerhans cell histiocytosis cells by their highly dendritic morphology, and thus rather resemble the MS-1+ macrophages in normal skin. RM 3/1 antigen shows a similar, but broader expression pattern including non-Langerhans cell histiocytoses, xanthelasmata palpebrarum, foreign body granulomas, granuloma annulare, and cellular type dermatofibroma. Moreover, xanthelasmata palpebrarum paradigmatically represent a class of macrophage lesions with strong RM 3/1, but little MS-1 antigen expression. In sarcoidosis, RM 3/1+ macrophages are only found at the very periphery of epithelioid cell granulomas. In contrast, 25F9 antigen is strongly and consistently expressed in epithelioid cells of sarcoidosis, and in foreign body granulomas. In cultured human monocytes/macrophages, RM 3/1 antigen is expressed early on, while MS-1 high molecular weight protein and 25F9 antigen are late and very late macrophage differentiation antigens, respectively. Expression of RM 3/1 antigen and MS-1 high molecular weight protein is inducible by glucocorticoid and interleukin-4, and less so by interleukin-13 and interleukin-10, and combinations thereof, while 25F9 antigen seems to be less influenced by these agents. Interferon-gamma (and less so tumor necrosis factor-alpha) inhibit expression of all three antigens in cultured human monocytes/macrophages.(ABSTRACT TRUNCATED AT 400 WORDS)
巨噬细胞在免疫和炎症以及过敏性、肉芽肿性和肿瘤性疾病中发挥着重要作用。在此,我们展示了一项正在进行的关于皮肤巨噬细胞疾病和体外巨噬细胞分化途径的深入研究结果。到目前为止,我们使用一组针对巨噬细胞分化抗原的单克隆和多克隆抗体(单克隆抗体MS-1、单克隆抗体α CD1a、单克隆抗体α CD34、单克隆抗体RM 3/1、单克隆抗体α CD11c、单克隆抗体α CD36、单克隆抗体MAC 387、单克隆抗体27E10、多克隆抗体α MRP-8和-14、单克隆抗体α CD68、单克隆抗体25F9、单克隆抗体DRC1-R4/23和单克隆抗体1F10)对总共40例皮肤巨噬细胞疾病(组织细胞增多症和肉芽肿)及相关疾病进行了检测。其中,MS-1高分子量蛋白由正常人器官中的非连续性窦状内皮细胞和高度树突状的血管周围巨噬细胞合成,是最具特异性的巨噬细胞分化标志物。MS-1高分子量蛋白在皮肤非朗格汉斯细胞组织细胞增多症中选择性表达,被证明是这些疾病的一种有价值的诊断工具。在朗格汉斯细胞组织细胞增多症细胞、结节病的上皮样细胞以及环状肉芽肿的栅栏状组织细胞中未发现MS-1高分子量蛋白。MS-1+巨噬细胞可能混杂存在于细胞型皮肤纤维瘤和异物肉芽肿中;它们与MS-1+非朗格汉斯细胞组织细胞增多症细胞的区别在于其高度树突状的形态,因此更类似于正常皮肤中的MS-1+巨噬细胞。RM 3/1抗原显示出类似但更广泛的表达模式,包括非朗格汉斯细胞组织细胞增多症、睑黄瘤、异物肉芽肿、环状肉芽肿和细胞型皮肤纤维瘤。此外,睑黄瘤典型地代表了一类具有强RM 3/1但MS-1抗原表达很少的巨噬细胞病变。在结节病中,RM 3/1+巨噬细胞仅在上皮样细胞肉芽肿的最外周发现。相比之下,25F9抗原在结节病的上皮样细胞和异物肉芽肿中强烈且持续表达。在培养的人单核细胞/巨噬细胞中,RM 3/1抗原早期表达,而MS-1高分子量蛋白和25F9抗原分别是晚期和极晚期巨噬细胞分化抗原。RM 3/1抗原和MS-1高分子量蛋白的表达可被糖皮质激素和白细胞介素-4诱导,而白细胞介素-13和白细胞介素-10及其组合的诱导作用较小,而25F9抗原似乎受这些因子的影响较小。干扰素-γ(肿瘤坏死因子-α的影响较小)抑制培养的人单核细胞/巨噬细胞中所有三种抗原的表达。(摘要截选至400字)
