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Emerging enzymatic targets controlling angiogenesis in cancer: preclinical evidence and potential clinical applications

机译:在癌症中控制血管生成的新出现酶促靶标:临床前证据和潜在的临床应用

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Angiogenesis has always been considered as a fundamental therapeutic target for inhibiting tumor growth and metastasis. To date, anti-angiogenic treatments that have been approved are principally based on either administration of monoclonal antibodies targeting the vascular endothelial growth factor/ vascular endothelial growth factor receptor axis or multikinase inhibitors. However, a growing body of evidence is pointing out the role of different classes of enzymes involved in tumor-driven angiogenesis, whose inhibition in preclinical models has already shown encouraging results. This review provides an overview on the current knowledge of potential enzymatic targets involved in tumor-driven angiogenesis and the potential clinical applications deriving from their modulation. Metalloproteinase and nitric oxide synthase inhibitors have been found to be, respectively, inefficacious or unsuitable for clinical applications. Conversely, early clinical studies evaluating the inhibition of heparanase, nicotinamide adenine dinucleotide phosphate (NADPH) oxidase, lysyl oxidase (LOX) and angiotensin-converting enzyme (ACE) have shown promising results. Therefore, preliminary evidence indicates that heparanase, NADPH oxidase, LOX and ACE might represent potential targets for anticancer therapy.
机译:血管生成一直被认为是抑制肿瘤生长和转移的基本治疗靶标。迄今为止,已批准的抗血管生成处理主要基于靶向血管内皮生长因子/血管内皮生长因子受体轴或多喹啉酶抑制剂的任一施用单克隆抗体。然而,越来越多的证据表明不同类别酶参与肿瘤驱动的血管生成的作用,其在临床前模型中的抑制已经显示出令人鼓舞的结果。本综述概述了关于肿瘤驱动血管生成中涉及的潜在酶促靶标的潜在酶促靶标的概况和潜在的临床应用。已经发现金属蛋白酶和一氧化氮合酶抑制剂,分别为临床应用,无效或不适合。相反,评估肝脏酶的抑制的早期临床研究,烟醇酰胺氨基磷酸酯(NADPH)氧化酶,赖氨酸氧化酶(LOX)和血管紧张素转换酶(ACE)的结果表明了有希望的结果。因此,初步证据表明乙酰肝素酶,NADPH氧化酶,LOX和ACE可能代表抗癌疗法的潜在目标。

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