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一种高分子量粘蛋白样抗原上多种肿瘤相关表位表达的可遗传变异。

Heritable variation in expression of multiple tumor associated epitopes on a high molecular weight mucin-like antigen.

作者信息

Linsley P S, Ochs V, Horn D, Ring D B, Frankel A E

出版信息

Cancer Res. 1986 Dec;46(12 Pt 1):6380-6.

PMID:2430697
Abstract

Monoclonal antibodies with specificity for mucin-like antigens have shown great promise for the diagnosis and therapy of human cancer. Heterogeneity in the expression of mucin-like antigens by tumor and normal cells has been noted in several previous studies. An understanding of the nature of this heterogeneity has important implications for the diagnostic and therapeutic usefulness of antibodies to mucin-like antigens. We have studied the mechanism of variability in expression of epitopes on a mucin-like antigen defined by monoclonal antibodies W1, W5, and W9 in the lung carcinoma cell line, Calu-1. Using the fluorescence activated cell sorter and clonal analysis, we have demonstrated that intercellular variability in mucin antigen expression by Calu-1 cells can be explained in part by heritable variation in the tumor cell population. Clonal cell lines were isolated which differ greatly in levels of epitopes for all three mucin directed antibodies. Levels of all three epitopes showed significant variation between different clonal lines but in general were coordinately regulated. Differences in epitope expression between two lines studied in detail could be attributed to a dramatic difference in expression of a high molecular weight mucin-like glycoprotein. In immunoblotting experiments the binding of all three antibodies to this glycoprotein was affected by sodium periodate and/or neuraminidase treatment, suggesting that the antibodies recognize carbohydrate epitopes. Thus, heterogeneity in expression of mucin-like glycoprotein antigens can result from heritable variations which affect expression of multiple carbohydrate epitopes.

摘要

对粘蛋白样抗原有特异性的单克隆抗体在人类癌症的诊断和治疗方面显示出巨大的前景。此前的几项研究已经注意到肿瘤细胞和正常细胞中粘蛋白样抗原表达的异质性。了解这种异质性的本质对于针对粘蛋白样抗原的抗体在诊断和治疗上的应用具有重要意义。我们研究了肺癌细胞系Calu-1中由单克隆抗体W1、W5和W9所定义的粘蛋白样抗原表位表达变异性的机制。利用荧光激活细胞分选仪和克隆分析,我们证明Calu-1细胞中粘蛋白抗原表达的细胞间变异性部分可以用肿瘤细胞群体中的遗传变异来解释。分离出的克隆细胞系对所有三种针对粘蛋白的抗体的表位水平差异很大。所有三种表位的水平在不同的克隆系之间显示出显著差异,但总体上是协同调节的。详细研究的两个细胞系之间表位表达的差异可归因于一种高分子量粘蛋白样糖蛋白表达的巨大差异。在免疫印迹实验中,所有三种抗体与这种糖蛋白的结合都受到高碘酸钠和/或神经氨酸酶处理的影响,这表明这些抗体识别碳水化合物表位。因此,粘蛋白样糖蛋白抗原表达的异质性可能源于影响多个碳水化合物表位表达的遗传变异。

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