Stein H, Mason D Y, Gerdes J, O'Connor N, Wainscoat J, Pallesen G, Gatter K, Falini B, Delsol G, Lemke H
Blood. 1985 Oct;66(4):848-58.
Ki-1 is a monoclonal antibody (raised against a Hodgkin's disease-derived cell line) that, in biopsy tissue affected by Hodgkin's disease, reacts selectively with Reed-Sternberg cells. The expression of Ki-1 antigen has been analyzed by immunocytochemical techniques in a wide range of human tissue and cell samples, including fetal tissue, malignant lymphomas (290 cases), and mitogen- and virus-transformed peripheral blood lymphocytes. The antigen was detectable on a variable proportion of cells in all cases of lymphomatoid papulosis and angio-immunoblastic lymphadenopathy and in 28% of the cases of peripheral T cell lymphomas (including lympho-epithelioid lymphomas). It was also expressed (more strongly) on tumor cells in 45 cases of diffuse large-cell lymphoma, most of which had originally been diagnosed as malignant histiocytosis or anaplastic carcinoma, because of their bizarre morphology. However, all of these cases lacked macrophage and epithelial antigens. Thirty-five cases expressed T cell-related antigens (associated in nine cases with the coexpression of B cell-related antigens), seven bore B cell-related antigens alone, and three were devoid of T and B cell markers. DNA hybridization with a JH specific probe showed a germline configuration in 11 cases of T cell phenotype, in two cases lacking T and B cell antigens, and in one case of mixed T/B phenotype, while rearrangement was found in two cases of clear B cell type and in one mixed T/B case. Expression of the Ki-1 antigen could be induced, together with interleukin 2 (IL 2) receptor, on normal lymphoid cells of both T and B cell type by exposure to phytohemagglutinin, human T leukemia viruses, Epstein-Barr virus, or Staphylococcus aureus. The results obtained indicate that Ki-1 antigen is an inducible lymphoid-associated molecule that identifies a group of hitherto poorly characterized normal and neoplastic large lymphoid cells. Tumors comprised solely of these cells show both morphological and immunological similarities to the neoplastic cells in Hodgkin's disease. This suggests that both disorders represent the neoplastic proliferation of activated lymphoid cells of either T cell or, less commonly, B cell origin. Disorders in which only a minority of cells express Ki-1 antigen (lymphomatoid papulosis, angio-immunoblastic lymphadenopathy, and certain T cell lymphomas) probably represent lesions in which only some of the abnormal cells have transformed into an "activation state." In direct support of this view is the finding that the Ki-1 expression in these lesions is accompanied by the expression of HLA-DR and IL 2 receptors.
Ki-1是一种单克隆抗体(针对源自霍奇金病的细胞系产生),在受霍奇金病影响的活检组织中,它能与里德-斯腾伯格细胞发生选择性反应。已通过免疫细胞化学技术在广泛的人体组织和细胞样本中分析了Ki-1抗原的表达情况,这些样本包括胎儿组织、恶性淋巴瘤(290例)以及丝裂原和病毒转化的外周血淋巴细胞。在所有淋巴瘤样丘疹病和血管免疫母细胞性淋巴结病病例以及28%的外周T细胞淋巴瘤病例(包括淋巴上皮样淋巴瘤)中,均可在不同比例的细胞上检测到该抗原。在45例弥漫性大细胞淋巴瘤的肿瘤细胞上也有表达(更强),其中大多数最初因形态怪异被诊断为恶性组织细胞增多症或间变性癌。然而,所有这些病例均缺乏巨噬细胞和上皮抗原。35例表达T细胞相关抗原(9例与B细胞相关抗原共表达),7例仅带有B细胞相关抗原,3例缺乏T和B细胞标志物。用JH特异性探针进行DNA杂交显示,11例T细胞表型病例、2例缺乏T和B细胞抗原的病例以及1例混合T/B表型病例中呈种系构型,而在2例明确的B细胞型病例和1例混合T/B病例中发现有重排。通过暴露于植物血凝素、人类T白血病病毒、爱泼斯坦-巴尔病毒或金黄色葡萄球菌,可在T和B细胞类型的正常淋巴细胞上诱导Ki-1抗原与白细胞介素2(IL-2)受体一起表达。所获得的结果表明,Ki-1抗原是一种可诱导的淋巴相关分子,可识别一组迄今特征不明的正常和肿瘤性大淋巴细胞。仅由这些细胞组成的肿瘤在形态和免疫方面与霍奇金病中的肿瘤细胞相似。这表明这两种疾病均代表T细胞起源或较少见的B细胞起源的活化淋巴细胞的肿瘤性增殖。只有少数细胞表达Ki-1抗原的疾病(淋巴瘤样丘疹病、血管免疫母细胞性淋巴结病和某些T细胞淋巴瘤)可能代表只有一些异常细胞已转变为 “活化状态” 的病变。直接支持这一观点的是,在这些病变中Ki-1表达伴随着HLA-DR和IL-2受体的表达。
