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Matrix metalloproteinase protein inhibitors: highlighting a new beginning for metalloproteinases in medicine

机译:基质金属蛋白酶蛋白抑制剂:突出了医学中金属蛋白酶的新起点

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The development of therapeutic matrix metalloproteinase (MMP) inhibitors has evolved from broad-spectrum peptidomimetic inhibitors with deleterious side effects, to highly selective agents. These range from small molecules to antibodies, antisense inhibitors, and engineered N-terminal tissue inhibitors of metalloproteinase domain. The advances in inhibitor design along with promising new global molecular insights into MMP structures, the protease web, and the role of extracellular matrix in diseases have contributed toward a renewed interest in using MMPs as valid drug targets. This review aims to address the advances and challenges concerning the design, development, and current status of anti-MMP agents in this new era of post-broad-spectrum MMP inhibitors. Highly selective inhibitors of MMPs promise to usher in an era of specific targeting of diseased tissue proteolysis networks, with markedly reduced negative repercussions, and to uncover the molecular and mechanistic roles of MMP isoforms in cancer, inflammation, and infection.
机译:治疗性基质金属蛋白酶(MMP)抑制剂的开发已从具有有害副作用的广谱拟肽抑制剂发展为高选择性试剂。这些范围从小分子到抗体,反义抑制剂和金属蛋白酶结构域的工程化N端组织抑制剂。抑制剂设计的进展以及对MMP结构,蛋白酶网以及细胞外基质在疾病中的作用的有希望的新的全球分子洞察力,促使人们重新将MMP用作有效的药物靶标。这篇综述旨在解决在广谱后MMP抑制剂新时代抗MMP药物的设计,开发和现状方面的进步和挑战。 MMPs的高度选择性抑制剂有望迎来一个特定靶向病变组织蛋白水解网络的时代,其负面影响显着减少,并揭示MMP亚型在癌症,炎症和感染中的分子和机制作用。

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