原位杂交
免疫组织化学
血管生成
病理
抗体
丛蛋白
生物
噬菌体展示
黑色素瘤
转移
癌症研究
平移(音频)
医学
癌症
免疫学
基因表达
信号灯
受体
基因
古生物学
镜头(地质)
生物化学
缩放
遗传学
作者
Ilse Roodink,Jos Raats,Bert van der Zwaag,Kiek Verrijp,Benno Küsters,Hans van Bokhoven,Marianne Linkels,Robert M.W. de Waal,William P. J. Leenders
出处
期刊:Cancer Research
[American Association for Cancer Research]
日期:2005-09-15
卷期号:65 (18): 8317-8323
被引量:67
标识
DOI:10.1158/0008-5472.can-04-4366
摘要
Abstract We previously reported that during mouse embryogenesis, plexin D1 (plxnD1) is expressed on neuronal and endothelial cells. Endothelial cells gradually loose plxnD1 expression during development. Here we describe, using in situ hybridization, that endothelial plxnD1 expression is regained during tumor angiogenesis in a mouse model of brain metastasis. Importantly, we found PLXND1 expression also in a number of human brain tumors, both of primary and metastatic origin. Apart from the tumor vasculature, abundant expression was also found on tumor cells. Via panning of a phage display library, we isolated two phages that carry single-domain antibodies with specific affinity towards a PLXND1-specific peptide. Immunohistochemistry with these single-domain antibodies on the same tumors that were used for in situ hybridization confirmed PLXND1 expression on the protein level. Furthermore, both these phages and the derived antibodies specifically homed to vessels in brain lesions of angiogenic melanoma in mice after i.v. injection. These results show that PLXND1 is a clinically relevant marker of tumor vasculature that can be targeted via i.v. injections.
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