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基质金属蛋白酶抑制作为一种新型抗癌策略:特别关注batimastat和marimastat的综述

Matrix metalloproteinase inhibition as a novel anticancer strategy: a review with special focus on batimastat and marimastat.

作者信息

Rasmussen H S, McCann P P

机构信息

British Biotech Inc., Annapolis, MD 21401, USA.

出版信息

Pharmacol Ther. 1997;75(1):69-75. doi: 10.1016/s0163-7258(97)00023-5.

Abstract

Matrix metalloproteinases (MMPs) are a homologous family of enzymes that are involved in tissue remodeling and morphogenesis. Collectively, these enzymes are capable of degrading all components of the extracellular matrix, and they play an important role in normal physiologic conditions, such as wound healing and other processes involving tissue remodeling. However, increased activity of these enzymes now has been observed in a number of different pathological conditions, and it has been hypothesized that such increased activity of MMPs might play a role in the pathogenesis of these conditions. Cancer is one such condition; extracellular matrices constitute the principal barrier to tumor growth and spread, and there is growing experimental evidence that malignant tumors utilize MMPs to overcome these barriers. Consequently, inhibitors of MMPs represent an attractive target for a new class of anticancer agents. Marimastat and batimastat are potent broad-spectrum inhibitors of all major MMPs and have been shown to prevent or reduce spread and growth of a number of different malignant tumors in numerous animal models. Both agents are now in advanced clinical testing in a number of different solid tumors in North America and Europe. The purpose of this paper is to review available preclinical and emerging clinical data, using batimastat and marimastat as prototype MMP inhibitors in the cancer area.

摘要

基质金属蛋白酶(MMPs)是一族同源酶,参与组织重塑和形态发生。这些酶共同作用能够降解细胞外基质的所有成分,并且在正常生理状况下发挥重要作用,如伤口愈合及其他涉及组织重塑的过程。然而,现已观察到在多种不同病理状况下这些酶的活性增加,并且据推测MMPs活性的这种增加可能在这些状况的发病机制中起作用。癌症就是这样一种状况;细胞外基质构成肿瘤生长和扩散的主要屏障,并且越来越多的实验证据表明恶性肿瘤利用MMPs来克服这些屏障。因此,MMPs抑制剂成为一类新型抗癌药物的有吸引力的靶点。马立马司他和batimastat是所有主要MMPs的强效广谱抑制剂,并且已证实在众多动物模型中可预防或减少多种不同恶性肿瘤的扩散和生长。目前这两种药物在北美和欧洲针对多种不同实体瘤正处于临床后期试验阶段。本文的目的是回顾现有的临床前和新出现的临床数据,将batimastat和马立马司他作为癌症领域MMP抑制剂的原型进行研究。

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