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长春地辛-单克隆抗体偶联物对人肿瘤细胞的选择性细胞毒性。

Selective cytotoxicity against human tumour cells by a vindesine-monoclonal antibody conjugate.

作者信息

Embleton M J, Rowland G F, Simmonds R G, Jacobs E, Marsden C H, Baldwin R W

出版信息

Br J Cancer. 1983 Jan;47(1):43-9. doi: 10.1038/bjc.1983.5.

Abstract

The anti-mitotic drug vindesine was coupled chemically to a monoclonal antibody raised originally against the human osteogenic sarcoma cell line, 791T. The cytotoxicity of the conjugate in vitro was tested, in comparison with free vindesine, against sarcoma 791T and other antigenically cross-reactive osteogenic sarcoma-cell lines, and also against tumour cell lines which have no detectable reaction with the monoclonal antibody. Continuous exposure of cultured 791T cells indicated that the vindesine was partially inactivated following conjugation since the conjugate was less toxic than the free drug. However, antibody-binding activity was essentially preserved following conjugation. Despite diminished drug activity in the conjugate, assays designed to mimic antibody binding to tumour in which target cells were treated with conjugate and washed before culture, showed selective cytotoxicity for osteogenic sarcoma lines with little or no effect on non-cross reactive control cells. In comparison, free vindesine was toxic equally for all cell lines and free antibody was non-toxic. These studies indicate that conjugation of a cytotoxic agent to a monoclonal antibody can confer on that agent selectivity for a particular target cell type which is recognised by the antibody.

摘要

抗有丝分裂药物长春地辛通过化学方法与一种最初针对人骨肉瘤细胞系791T产生的单克隆抗体偶联。与游离长春地辛相比,测试了该偶联物对肉瘤791T和其他抗原交叉反应性骨肉瘤细胞系的体外细胞毒性,还测试了其对与该单克隆抗体无可检测反应的肿瘤细胞系的细胞毒性。对培养的791T细胞的持续暴露表明,偶联后长春地辛部分失活,因为偶联物的毒性低于游离药物。然而,偶联后抗体结合活性基本保留。尽管偶联物中的药物活性降低,但在模拟抗体与肿瘤结合的试验中,先用偶联物处理靶细胞并在培养前洗涤,结果显示对骨肉瘤细胞系具有选择性细胞毒性,对非交叉反应性对照细胞几乎没有影响。相比之下,游离长春地辛对所有细胞系均有毒性,游离抗体则无毒性。这些研究表明,将细胞毒性剂与单克隆抗体偶联可赋予该剂对抗体识别的特定靶细胞类型的选择性。

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