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作为肿瘤血管靶向剂的考布他汀生物学特性。

The biology of the combretastatins as tumour vascular targeting agents.

作者信息

Tozer Gillian M, Kanthou Chryso, Parkins Charles S, Hill Sally A

机构信息

Gray Cancer Institute, PO Box 100, Mount Vernon Hospital, Northwood, Middlesex HA6 2JR, UK.

出版信息

Int J Exp Pathol. 2002 Feb;83(1):21-38. doi: 10.1046/j.1365-2613.2002.00211.x.

Abstract

The tumour vasculature is an attractive target for therapy. Combretastatin A-4 (CA-4) and A-1 (CA-1) are tubulin binding agents, structurally related to colchicine, which induce vascular-mediated tumour necrosis in animal models. CA-1 and CA-4 were isolated from the African bush willow, Combretum caffrum, and several synthetic analogues are also now available, such as the Aventis Pharma compound, AVE8062. More soluble, phosphated, forms of CA-4 (CA-4-P) and CA-1 (CA-1-P) are commonly used for in vitro and in vivo studies. These are cleaved to the natural forms by endogenous phosphatases and are taken up into cells. The lead compound, CA-4-P, is currently in clinical trial as a tumour vascular targeting agent. In animal models, CA-4-P causes a prolonged and extensive shut-down of blood flow in established tumour blood vessels, with much less effect in normal tissues. This paper reviews the current understanding of the mechanism of action of the combretastatins and their therapeutic potential.

摘要

肿瘤血管系统是一个有吸引力的治疗靶点。康普瑞他汀A - 4(CA - 4)和A - 1(CA - 1)是微管蛋白结合剂,其结构与秋水仙碱相关,在动物模型中可诱导血管介导的肿瘤坏死。CA - 1和CA - 4是从非洲灌木柳树Combretum caffrum中分离出来的,现在也有几种合成类似物,如安万特制药公司的化合物AVE8062。更易溶的磷酸化形式的CA - 4(CA - 4 - P)和CA - 1(CA - 1 - P)常用于体外和体内研究。它们被内源性磷酸酶裂解为天然形式并被细胞摄取。先导化合物CA - 4 - P目前作为一种肿瘤血管靶向剂正在进行临床试验。在动物模型中,CA - 4 - P可导致已建立的肿瘤血管中血流长时间广泛阻断,而对正常组织的影响则小得多。本文综述了目前对康普瑞他汀作用机制及其治疗潜力的认识。

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