Structure of solid tumors and their vasculature: implications for therapy with monoclonal antibodies.

IF 3.5 Q1 DENTISTRY, ORAL SURGERY & MEDICINE Cancer cells (Cold Spring Harbor, N.Y. : 1989) Pub Date : 1991-03-01
H F Dvorak, J A Nagy, A M Dvorak
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Abstract

Delivery of monoclonal antibodies to solid tumors is a vexing problem that must be solved if these antibodies are to realize their promise in therapy. Such success as has been achieved with monoclonal antibodies is attributable to the local hyperpermeability of the tumor vasculature, a property that favors antibody extravasation at tumor sites and that is mediated by a tumor-secreted vascular permeability factor. However, leaky tumor blood vessels are generally some distance removed from target tumor cells, separated by stroma and by other tumor cells that together represent significant barriers to penetration by extravasated monoclonal antibodies. For this reason, alternative approaches may be attractive. These include the use of antibody-linked cytotoxins, which are able to kill tumor cells without immediate contact, and direction of antibodies against nontumor cell targets, for example, antigens unique to the tumor vascular endothelium or to tumor stroma.

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实体瘤的结构及其血管系统:单克隆抗体治疗的意义。
单克隆抗体的实体瘤递送是一个棘手的问题,必须解决,如果这些抗体是实现其在治疗中的承诺。单克隆抗体取得的这种成功归因于肿瘤血管的局部高渗透性,这种特性有利于抗体在肿瘤部位外渗,并由肿瘤分泌的血管渗透性因子介导。然而,渗漏的肿瘤血管通常与靶肿瘤细胞有一定距离,被基质和其他肿瘤细胞隔开,这些细胞共同构成了外渗的单克隆抗体渗透的重大障碍。出于这个原因,其他方法可能更有吸引力。这些方法包括使用抗体连接的细胞毒素,它能够在不直接接触肿瘤细胞的情况下杀死肿瘤细胞,以及使用针对非肿瘤细胞目标的抗体,例如肿瘤血管内皮或肿瘤基质所特有的抗原。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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