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PL-09 side effects of anti-angiogenic drugs

机译:PL-09抗血管生成药物的副作用

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Anti-angiogenic drugs and in particular anti-vascular endothelial growth factor (VEGF) agents have entered the clinical armamentarium against cancer. New unexpected toxicities have emerged. The incidence and the severity of these toxicities have a great variability in the different studies. Among them, bleeding is one of the most severe and difficult to manage. Bevacizumab retains the highest frequency of bleeding complications, in particular epistaxis, hemoptysis and gastrointestinal bleeding. Although a higher incidence of severe hemorrhages has not been consistently demonstrated during the treatment with bevacizumab, mild bleeding episodes appear clearly increased in the experimental arm of most trials. Cases of severe pulmonary hemorrhage were reported in patients with lung cancer; these events occurred mainly intra-tumor and were significantly associated with squamous cell histology. Trials with other small-molecule tyrosine kinase inhibitors like sunitinib or sorafenib showed an overall lower rate of bleeding complications, but still significantly higher than the control arm in many cases. The mechanisms of bleeding induced by anti-VEGF agents are complex and not yet fully clarified: the main hypothesis is that VEGF could promote endothelial cell survival and integrity in the adult vasculature and its inhibition may decrease the renewal capacity of damaged endothelial cells. Management of bleeding in patients treated with anti-VEGF agents is a challenging task because this complication is at least in part inherent to the efficacy of the drug and because there is also an increased risk of thrombosis, both arterial and venous. So far, only few preliminary data are available on a strategy to prevent hemorrhage and thrombotic event.
机译:抗血管生成药物,尤其是抗血管内皮生长因子(VEGF)药物已进入临床抗癌药库。新的意外毒性已经出现。在不同的研究中,这些毒性的发生率和严重性差异很大。其中,出血是最严重,最难处理的出血之一。贝伐单抗保留了最高的出血并发症发生率,尤其是鼻出血,咯血和胃肠道出血。尽管在用贝伐单抗治疗期间未始终证明严重出血的发生率较高,但在大多数试验的实验组中,轻度出血事件似乎明显增加。肺癌患者中报告了严重的肺出血病例。这些事件主要发生在肿瘤内,并且与鳞状细胞组织学显着相关。使用其他小分子酪氨酸激酶抑制剂(如舒尼替尼或索拉非尼)的试验显示出血并发症的总体发生率较低,但在许多情况下仍显着高于对照组。由抗VEGF剂引起的出血的机制很复杂,尚未完全阐明:主要假说是VEGF可以促进成年脉管系统中内皮细胞的存活和完整性,而其抑制作用可能会降低受损内皮细胞的更新能力。用抗VEGF药物治疗患者的出血管理是一项艰巨的任务,因为这种并发症至少部分是药物疗效所固有的,并且还增加了动脉和静脉血栓形成的风险。到目前为止,只有很少的初步数据可用于预防出血和血栓形成事件。

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