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通过羧甲基葡聚糖与抗肿瘤抗体复合的顺铂对肿瘤细胞的选择性细胞毒性。

Selective cytotoxicity against tumor cells by cisplatin complexed to antitumor antibodies via carboxymethyl dextran.

作者信息

Schechter B, Pauzner R, Arnon R, Haimovich J, Wilchek M

机构信息

Department of Chemical Immunology, Weizmann Institute of Science, Rehovot, Israel.

出版信息

Cancer Immunol Immunother. 1987;25(3):225-30. doi: 10.1007/BF00199151.

Abstract

Cis-diamminedichloroplatinum (II) (cis-DDP) and its structural analogue cis-diamminediaquoplatinum(II) nitrate (cis-aq) were complexed via an intermediate dextran carrier to antibodies specifically reactive with B lymphoma cells (38C-13). The potential use of these drugs in site-directed immunotargeting was evaluated. The two platinum(II) compounds were previously shown to form pharmacologically active complexes with carboxymethyl dextran (CM-dex). For the purpose of preparing drug-antibody complexes, CM-dex was first conjugated to idiotypic antibodies that recognize a specific membrane IgM on the B lymphoma cells. The conjugates were prepared by a modified water-soluble carbodiimide method in which N-hydroxysuccinimide was used to enhance the coupling reaction. The conjugation was followed by separation of the CM-dex-IgG conjugates from unconjugated CM-dex or IgG. The platinum(II) compounds were then complexed to the CM-dex-IgG resulting in complexes carrying up to 50 mole drug/mole IgG. Both cis-DDP and cis-aq complexes of CM-dex-antibody conjugates maintained most of the original cell-binding activity of the antibodies. An in vitro assay was used to demonstrate selective binding to tumor cells in which the target cells were treated with specific immune complexes and washed before culture. In this assay the specific complexes showed preferential cytotoxicity for the B lymphoma cells in comparison to the free drugs, drug CM-dex, or nonspecific immune complexes.

摘要

顺二氯二氨铂(II)(顺铂)及其结构类似物顺二氨二水铂(II)硝酸盐(顺式水合物)通过中间葡聚糖载体与对B淋巴瘤细胞(38C - 13)具有特异性反应的抗体复合。评估了这些药物在定点免疫靶向中的潜在用途。先前已证明这两种铂(II)化合物可与羧甲基葡聚糖(CM - 葡聚糖)形成药理活性复合物。为了制备药物 - 抗体复合物,首先将CM - 葡聚糖与识别B淋巴瘤细胞上特定膜IgM的独特型抗体偶联。通过改良的水溶性碳二亚胺方法制备偶联物,其中使用N - 羟基琥珀酰亚胺来增强偶联反应。偶联后,将CM - 葡聚糖 - IgG偶联物与未偶联的CM - 葡聚糖或IgG分离。然后将铂(II)化合物与CM - 葡聚糖 - IgG复合,得到每摩尔IgG携带多达50摩尔药物的复合物。CM - 葡聚糖 - 抗体偶联物的顺铂和顺式水合物复合物均保持了抗体大部分原始的细胞结合活性。使用体外试验来证明对肿瘤细胞的选择性结合,其中用特异性免疫复合物处理靶细胞并在培养前洗涤。在该试验中,与游离药物、药物CM - 葡聚糖或非特异性免疫复合物相比,特异性复合物对B淋巴瘤细胞显示出优先的细胞毒性。

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