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识别神经细胞黏附分子的弱活性蓖麻毒素A链免疫毒素的增强作用

Potentiation of a weakly active ricin A chain immunotoxin recognizing the neural cell adhesion molecule.

作者信息

Derbyshire E J, Stahel R A, Wawrzynczak E J

机构信息

Drug Targeting Laboratory, Section of Immunology, Institute of Cancer Research, Sutton, UK.

出版信息

Clin Exp Immunol. 1992 Sep;89(3):336-40. doi: 10.1111/j.1365-2249.1992.tb06958.x.

Abstract

A ricin A chain immunotoxin, SEN36-ricin A chain, directed against the neural cell adhesion molecule (N-CAM) had no selective cytotoxic activity against three different small cell lung cancer (SCLC) cell lines in tissue culture despite expression of the target antigen on more than 98% of cells in each line detected by indirect immunofluorescence. Treatment of the SW2 SCLC cell line with suramin and interferons alpha and gamma increased the level of N-CAM expression only slightly and had no significant effect on the cytotoxic activity of the SEN36 immunotoxin. In the presence of the carboxylic ionophore monensin at a concentration of 0.1 microM, the toxicity of SEN36-ricin A chain to the SW2 cell line was enhanced by 12,000-fold. In contrast, lysosomotropic amines showed little or no potentiation of activity, suggesting that lysosomal degradation was not the major factor limiting the action of the anti-N-CAM immunotoxin. The findings of this study indicate that ricin A chain immunotoxins directed against N-CAM on SCLC are unlikely to have sufficient activity to be useful therapeutic agents in the absence of potentiating agents such as monensin, which can interfere with the normal intracellular pathways of antigen routing.

摘要

一种针对神经细胞黏附分子(N-CAM)的蓖麻毒素A链免疫毒素SEN36-蓖麻毒素A链,尽管通过间接免疫荧光检测发现每种细胞系中超过98%的细胞表达靶抗原,但在组织培养中对三种不同的小细胞肺癌(SCLC)细胞系没有选择性细胞毒性活性。用苏拉明以及α和γ干扰素处理SW2小细胞肺癌细胞系,仅略微增加了N-CAM的表达水平,并且对SEN36免疫毒素的细胞毒性活性没有显著影响。在浓度为0.1微摩尔的羧酸离子载体莫能菌素存在下,SEN36-蓖麻毒素A链对SW2细胞系的毒性增强了12000倍。相比之下,溶酶体促渗胺对活性几乎没有增强作用,这表明溶酶体降解不是限制抗N-CAM免疫毒素作用的主要因素。本研究结果表明,在没有如莫能菌素等能干扰抗原正常细胞内转运途径的增效剂的情况下,针对小细胞肺癌上N-CAM的蓖麻毒素A链免疫毒素不太可能具有足够的活性成为有用的治疗剂。

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Clin Exp Immunol. 1992 Sep;89(3):336-40. doi: 10.1111/j.1365-2249.1992.tb06958.x.

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