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儿童淋巴瘤复发时骨髓及髓外细胞膜抗原表达的变化

Bone marrow and extramedullary variations of cell membrane antigen expression in childhood lymphoid neoplasias at relapse.

作者信息

Lauer S, Piaskowski V, Camitta B, Casper J

出版信息

Leuk Res. 1982;6(6):769-74. doi: 10.1016/0145-2126(82)90058-3.

Abstract

To increase our knowledge of the pathogenesis of tumour recurrence, cell membrane phenotypes were determined on bone marrow and extramedullary tumour cells at diagnosis and at relapse in 24 children with lymphoid malignancies. There were 19 patients with acute lymphoblastic leukemia and five with non-Hodgkin's lymphoma. Membrane characteristics used for classification were E-rosetting, T antigen, surface immunoglobulin (sIg) and Ia antigen. Twelve patients were phenotyped as non-T, non-B, five as T-like and seven as B-like leukemia/lymphoma. Eighty-eight tissue samples were assayed for cell surface markers at the time of relapse(s). Lymphoblasts from 18 children (75%) demonstrated no variation in membrane marker expression. Six patients (25%) showed alteration of antigen expression on lymphoblasts obtained during relapses. This was manifested by loss of Ia antigen in two patients, loss of E-rosetting in one patient and loss of sIgD in one patient. Lymphoblasts from two patients, initially non-reactive with the four membrane markers utilized, expressed Ia antigen on subsequent relapses. Despite these variations no patient was categorized differently (i.e. T-like becoming non-T, non-B). Simultaneous lymphoblast phenotype determination from multiple body sites in 13 children showed no variation in marker analysis. A lymphoblast's phenotype remains stable throughout repeated relapses and is not influenced by relapse site in most children with lymphoid neoplasias. This information may be helpful in designing protocols where cytotoxic monoclonal antibodies are used as a treatment modality in patients with recurrent disease.

摘要

为了增进我们对肿瘤复发发病机制的了解,我们测定了24例淋巴系统恶性肿瘤患儿在诊断时和复发时骨髓及髓外肿瘤细胞的细胞膜表型。其中19例为急性淋巴细胞白血病患者,5例为非霍奇金淋巴瘤患者。用于分类的膜特征包括E玫瑰花结形成、T抗原、表面免疫球蛋白(sIg)和Ia抗原。12例患者的表型为非T、非B,5例为T样,7例为B样白血病/淋巴瘤。在复发时对88份组织样本进行了细胞表面标志物检测。18名儿童(75%)的淋巴母细胞在膜标志物表达上没有变化。6例患者(25%)在复发时获得的淋巴母细胞上显示出抗原表达的改变。这表现为2例患者Ia抗原缺失,1例患者E玫瑰花结形成缺失,1例患者sIgD缺失。2例患者的淋巴母细胞最初对所使用的四种膜标志物无反应,但在随后的复发中表达了Ia抗原。尽管存在这些变化,但没有患者被重新分类(即T样变为非T、非B)。对13名儿童多个身体部位的淋巴母细胞表型进行同时测定,结果显示标志物分析没有变化。在大多数淋巴系统肿瘤患儿中,淋巴母细胞的表型在反复复发过程中保持稳定,且不受复发部位的影响。这些信息可能有助于设计将细胞毒性单克隆抗体用作复发性疾病患者治疗方式的方案。

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