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The Rebirth of Matrix Metalloproteinase Inhibitors: Moving Beyond the Dogma

机译:基质金属蛋白酶抑制剂的重生:超越教条

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摘要

The pursuit of matrix metalloproteinase (MMP) inhibitors began in earnest over three decades ago. Initial clinical trials were disappointing, resulting in a negative view of MMPs as therapeutic targets. As a better understanding of MMP biology and inhibitor pharmacokinetic properties emerged, it became clear that initial MMP inhibitor clinical trials were held prematurely. Further complicating matters were problematic conclusions drawn from animal model studies. The most recent generation of MMP inhibitors have desirable selectivities and improved pharmacokinetics, resulting in improved toxicity profiles. Application of selective MMP inhibitors led to the conclusion that MMP-2, MMP-9, MMP-13, and MT1-MMP are not involved in musculoskeletal syndrome, a common side effect observed with broad spectrum MMP inhibitors. Specific activities within a single MMP can now be inhibited. Better definition of the roles of MMPs in immunological responses and inflammation will help inform clinic trials, and multiple studies indicate that modulating MMP activity can improve immunotherapy. There is a U.S. Food and Drug Administration (FDA)-approved MMP inhibitor for periodontal disease, and several MMP inhibitors are in clinic trials, targeting a variety of maladies including gastric cancer, diabetic foot ulcers, and multiple sclerosis. It is clearly time to move on from the dogma of viewing MMP inhibition as intractable.
机译:三十年前,追求基质金属蛋白酶(MMP)抑制剂始于恳切。初步临床试验令人失望,导致MMP的负面观作为治疗目标。作为对MMP生物学和抑制剂药代动力学性质的更好理解,它很明显,初始MMP抑制剂临床试验过早地保持。从动物模型研究中汲取的进一步复杂性问题是有问题的结论。最近一代MMP抑制剂具有理想的选择性和改善的药代动力学,导致毒性谱改善。选择性MMP抑制剂的应用导致了MMP-2,MMP-9,MMP-13和MT1-MMP不参与肌肉骨骼综合征的结论,用广谱MMP抑制剂观察到常见的副作用。现在可以抑制单一MMP的特定活动。更好地定义MMP在免疫反应和炎症中的角色将有助于通知诊所试验,并且多项研究表明调节MMP活性可以改善免疫疗法。有一个美国食品和药物管理局(FDA) - 批准的MMP抑制剂用于牙周病,几种MMP抑制剂在临床试验中,靶向各种疾病,包括胃癌,糖尿病足溃疡和多发性硬化。显然是时候从观察MMP抑制作为棘手的教条中移动。

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    Gregg B. Fields;

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  • 年度 2019
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  • 原文格式 PDF
  • 正文语种 eng
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