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对多种抗人腺癌细胞的抗癌胚抗原免疫毒素的比较。

Comparison of multiple anti-CEA immunotoxins active against human adenocarcinoma cells.

作者信息

Levin L V, Griffin T W, Childs L R, Davis S, Haagensen D E

出版信息

Cancer Immunol Immunother. 1987;24(3):202-6. doi: 10.1007/BF00205630.

Abstract

Anti-carcinoembryonic antigen (CEA) immunotoxins constructed with multiple anti-CEA antibodies (goat and baboon polyclonal, and three murine monoclonal antibodies) by covalently linking them to the A chain of ricin via a disulfide bond all function as potent and specific toxins for CEA-bearing cells, suggesting that the CEA molecule is capable of directing productive internalization of ricin A chain. The high potency of anti-CEA immunotoxins apparently makes addition of ricin B chain unnecessary for high toxic efficiency, as in some other systems, because presence of the B chain reduces target cell specificity. Several characteristics of the immunotoxins which might account for their cytotoxic potency were studied. Equilibrium association constants of the goat, baboon, and murine monoclonal C-19 antibodies with fluid-phase CEA were determined by using Langmuir plots and were found to be 8.79, 6.61, and 8.13 X 10(9) M-1, respectively, indicating the high and similar affinities of the three antibodies toward CEA. Radioimmunoassay binding studies of the three immunotoxins with 125I-CEA showed that the antibody portions of the molecules retained the ability to form complexes with CEA after conjugation to ricin A chain. The maximum number of anti-CEA antibody molecules bound per cell, as demonstrated by 111In-labeled C-19 binding assays with CEA-bearing cell lines, varied from 2.65 X 10(5) per cell for HT29 to 2.01 X 10(6) for LoVo, with an intermediate value of 1.17 X 10(6) per cell for WiDr. Cytotoxicity of the immunotoxins was assessed by inhibition of protein synthesis and expressed as a median inhibitory dose (ID50). Comparison of the ID50's of each immunotoxin on the three cell lines has shown that the immunotoxin made of the monoclonal C-19 antibody is in general 6 to 7 times more cytotoxic than the goat and baboon antibody immunotoxins. The affinity of CEA-antibody binding is probably an important, but not a sole factor in determining the immunotoxin potency. The fact that the antibodies with very similar affinity toward fluid phase CEA make immunotoxins of different potency might indicate that interactions with membrane-bound CEA are more complex and/or the efficiency of internalization of various immunotoxins is different. An important factor in immunotoxin action appears to be the CEA content in target adenocarcinoma cells.

摘要

用多种抗癌胚抗原(CEA)抗体(山羊和狒狒多克隆抗体以及三种鼠单克隆抗体)通过二硫键将它们与蓖麻毒素A链共价连接构建的抗CEA免疫毒素,对表达CEA的细胞均起高效特异性毒素的作用,这表明CEA分子能够引导蓖麻毒素A链进行有效的内化。抗CEA免疫毒素的高效性显然使得像其他一些系统那样添加蓖麻毒素B链以获得高毒性效率变得不必要,因为B链的存在会降低靶细胞特异性。对可能解释其细胞毒性效力的免疫毒素的几个特性进行了研究。通过使用朗缪尔图测定山羊、狒狒和鼠单克隆C-19抗体与液相CEA的平衡缔合常数,发现分别为8.79、6.61和8.13×10⁹ M⁻¹,表明这三种抗体对CEA具有高且相似的亲和力。三种免疫毒素与¹²⁵I-CEA的放射免疫分析结合研究表明,分子的抗体部分在与蓖麻毒素A链偶联后仍保留与CEA形成复合物的能力。用¹¹¹In标记的C-19与表达CEA的细胞系进行结合测定表明,每个细胞结合的抗CEA抗体分子的最大数量各不相同,从HT29细胞的每个细胞2.65×10⁵个到LoVo细胞的每个细胞2.01×10⁶个不等,WiDr细胞的中间值为每个细胞1.17×10⁶个。通过抑制蛋白质合成评估免疫毒素的细胞毒性,并表示为半数抑制剂量(ID50)。每种免疫毒素在三种细胞系上的ID50比较表明,由单克隆C-19抗体制成的免疫毒素的细胞毒性通常比山羊和狒狒抗体免疫毒素高6至7倍。CEA - 抗体结合的亲和力可能是决定免疫毒素效力的一个重要但非唯一因素。对液相CEA亲和力非常相似的抗体产生不同效力的免疫毒素这一事实可能表明,与膜结合CEA的相互作用更为复杂和/或各种免疫毒素的内化效率不同。免疫毒素作用的一个重要因素似乎是靶腺癌细胞中的CEA含量。

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