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用于癌症治疗的基质金属蛋白酶抑制剂:现状与未来展望

Matrix metalloproteinase inhibitors for cancer therapy:the current situation and future prospects.

作者信息

Fingleton Barbara

机构信息

Vanderbilt University Medical Center, Department of Cancer Biology, 736 PRB 23rd and Pierce Avenues, Nashville, TN 37232-6840, USA.

出版信息

Expert Opin Ther Targets. 2003 Jun;7(3):385-97. doi: 10.1517/14728222.7.3.385.

Abstract

Inhibition of matrix metalloproteinases (MMPs), a family of proteolytic enzymes linked to many aspects of cancer progression, has been explored as a therapeutic goal for almost two decades. Thus far, all tested MMP inhibitors (MMPIs) have failed to reach primary end points in Phase III clinical trials, although secondary analyses suggest benefits in particular patient groups. The clinical development of these agents has been hampered by problems related to determination of effective dosages and side effects that necessitate dose lowering or drug holidays. Imaging technologies offer hope as a means to measure enzyme activity and hence effective enzyme inhibition in vivo. Meanwhile, recent results from genetic studies of both mice and man have given some clues to possible causes of musculoskeletal side effects. Future progress in the therapeutic use of MMPIs is dependent on the ability to selectively target cancer-associated MMPs at the correct stage in tumour progression and the development of surrogate markers of in vivo efficacy.

摘要

基质金属蛋白酶(MMPs)是一族与癌症进展诸多方面相关的蛋白水解酶,近二十年来,抑制MMPs一直被作为一个治疗目标来探索。迄今为止,所有经测试的MMP抑制剂(MMPIs)在III期临床试验中均未达到主要终点,尽管二次分析表明在特定患者群体中存在益处。这些药物的临床开发受到与有效剂量确定及副作用相关问题的阻碍,这些问题使得必须降低剂量或停药。成像技术有望成为一种在体内测量酶活性从而测定有效酶抑制作用的手段。同时,小鼠和人类的遗传学研究近期结果为肌肉骨骼副作用的可能成因提供了一些线索。MMPIs治疗应用的未来进展取决于在肿瘤进展的正确阶段选择性靶向癌症相关MMPs的能力以及体内疗效替代标志物的开发。

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