首页> 外文期刊>Journal of Immunological Methods >Isolation of human antibodies to tumor-associated endothelial cell markers by in vitro human endothelial cell selection with phage display libraries.
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Isolation of human antibodies to tumor-associated endothelial cell markers by in vitro human endothelial cell selection with phage display libraries.

机译:通过噬菌体展示文库的体外人内皮细胞选择,分离针对肿瘤相关内皮细胞标记物的人抗体。

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摘要

Human antibodies selectively targeting angiogenic vessels hold great promise for the immunotherapy of human malignancies and can help to elucidate the molecular mechanisms regulating angiogenesis. By selecting a large antibody phage display library on proliferating stimulated HUVEC, we have isolated 15 human antibodies that bind to HUVEC in flow cytometric analysis, 11 of which target the vasculature of colorectal carcinomas as demonstrated by immunohistochemical analysis. The four most specific antibodies, TEM-A, TEM-C, TEM-M and TEM-Q, also stain the vasculature of a series of carcinomas derived from liver, ovary, kidney, bladder, lung and breast, and either react weakly or not all with the vasculature of corresponding normal tissues. All four antibodies react with the vasculature of endometrium, but only TEM-M and TEM-Q react with the vasculature of placenta. As shown by non-reducing western blot analysis, 9/15 of the antibodies recognize either one or two distinct bands on HUVEC cell lysates, with molecular weights of 175 and/or 110-125 kDa. Antibodies identified by this approach may be used for the identification of new markers of angiogenesis and/or tumor vasculature. The selected antibodies may prove useful as new prognostic markers, for in vivo tumor imaging purposes and for further development of targeted therapies.
机译:选择性靶向血管生成血管的人类抗体在人类恶性肿瘤的免疫治疗中具有广阔的前景,并可帮助阐明调节血管生成的分子机制。通过选择关于刺激的HUVEC增殖的大型抗体噬菌体展示文库,我们在流式细胞仪分析中分离了15种与HUVEC结合的人抗体,其中11种针对大肠癌的血管,如免疫组织化学分析所示。四种最特异的抗体TEM-A,TEM-C,TEM-M和TEM-Q也染色了一系列源自肝,卵巢,肾,膀胱,肺和乳腺癌的癌的脉管系统,它们的反应较弱或并非全部具有相应正常组织的脉管系统。所有四种抗体均与子宫内膜的血管反应,但只有TEM-M和TEM-Q与胎盘的血管反应。如非还原蛋白质印迹分析所示,9/15的抗体可识别分子量为175和/或110-125 kDa的HUVEC细胞裂解物上的一个或两个不同的条带。通过这种方法鉴定的抗体可以用于鉴定血管生成和/或肿瘤脉管系统的新标记。所选择的抗体可被证明是新的预后标志物,可用于体内肿瘤成像和进一步开发靶向疗法。

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