一种针对人乳腺癌的含有胶质蛋白的免疫毒素。

Molecular biotherapy Pub Date : 1992-09-01
M G Rosenblum, J E Zuckerman, J W Marks, J Rotbein, W R Allen
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引用次数: 0

摘要

毒素可以特异性地靶向肿瘤细胞,并且通过与识别肿瘤相关抗原的单克隆抗体的共价偶联,毒素的效力大大增加。免疫球蛋白G1 (IgG1)亚类抗人乳腺癌小鼠单克隆抗体15A8和植物毒素gelonin分别与n -琥珀酰3-(2-吡喃二硫代)本体酸酯和亚氨基硫代烷共价修饰,并允许交联。从未反应抗体和游离明胶蛋白中通过凝胶过滤和蓝葡聚糖层析纯化出15a8 -明胶蛋白偶联物。经十二烷基硫酸钠-聚丙烯酰胺凝胶电泳分析,最终产物含有两条与抗体对应的条带:凝胶蛋白偶联物1:1(优势)和1:2。制备过程中未发现游离抗体和游离毒素污染量。根据起始抗体的量,最终纯化的15A8-gelonin偶联物的产率约为20%。免疫偶联物的蛋白合成抑制活性通过体外兔网织细胞翻译试验进行评价。这种功能活性与未修饰的gelonin标准化,用于抗原阴性(Hs294t人黑色素瘤)和抗原阳性(ME-180人宫颈癌)细胞系的体外抗增殖试验。抗原阴性的Hs294t细胞与15A8-gelonin免疫毒素孵育72小时后,与单独暴露于游离gelonin的Hs294t细胞相比,细胞毒性没有增加。然而,免疫毒素对抗原阳性的ME-180细胞具有优先毒性;15A8-gelonin暴露72小时后,观察到的细胞死亡比单独暴露相同gelonin后的细胞死亡多5倍。各种促溶体剂增强15a8 -凝胶蛋白的细胞毒性;最有效的增强剂似乎是莫能菌素。此外,化疗药物l -苯丙氨酸芥(L-PAM)、5-氟尿嘧啶、长春新碱和博来霉素,以及生物反应调节剂干扰素- α和肿瘤坏死因子- α被证明可以增强15A8-gelonin的细胞毒性。如果体内药理学和治疗研究证实了这些体外研究结果,15A8-gelonin偶联物可能是治疗人类癌症的有效药物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A gelonin-containing immunotoxin directed against human breast carcinoma.

Toxins may be specifically directed to tumor cells and the toxins' potency greatly increased by covalent conjugation to monoclonal antibodies recognizing tumor-associated antigens. Antibody 15A8, an immunoglobulin G1 (IgG1) subclass anti-human breast carcinoma murine monoclonal antibody and gelonin, a plant toxin, were covalently modified with N-succimindyl 3-(2-pyridyldithio) proprionate and iminothiolane, respectively, and allowed to cross-link. 15A8-gelonin conjugates were purified from unreacted antibody and free gelonin by gel filtration and blue sepharose chromatography. Analysis by sodium dodecyl sulfate-polyacrylamide gel electrophoresis showed that the final product contained two bands corresponding to antibody:gelonin conjugates of 1:1 (predominant) and 1:2. There were no contaminating amounts of free antibody or free toxin in the preparation. The yield of the final purified 15A8-gelonin conjugate was approximately 20% based on the amount of starting antibody. The protein synthesis inhibitory activity of the immunoconjugate was assessed by in vitro rabbit reticulocyte translation assay. This functional activity was normalized to that of unmodified gelonin for use in in vitro antiproliferative assays against antigen-negative (Hs294t human melanoma) and antigen-positive (ME-180 human cervical carcinoma) cell lines. Antigen-negative Hs294t cells incubated for 72 hours with 15A8-gelonin immunotoxin showed no increased cytotoxicity compared with HS294t cells exposed to free gelonin alone. However, the immunotoxin was preferentially toxic to antigen-positive ME-180 cells; over 5 logs greater cell kill was observed after 72 hours exposure to 15A8-gelonin than after the same exposure to gelonin alone. Various lysosomotropic agents augmented 15A8-gelonin cytotoxicity; the most effective potentiating agent appeared to be monensin. In addition, the chemotherapeutic agents L-phenylalanine mustard (L-PAM), 5-fluorouracil, vincristine, and bleomycin, and the biological response modifiers interferon-alpha and tumor necrosis factor-alpha were shown to augment 15A8-gelonin cytotoxicity. Should in vivo pharmacology and therapeutic studies confirm these in vitro findings, 15A8-gelonin conjugate may be a potent agent for therapy of cancer in man.

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