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Anti-angiogenic Therapy in Cancer: Downsides and New Pivots for Precision Medicine

机译:癌症的抗血管生成治疗:精密医学的弊端和新思路

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摘要

Primary solid tumors originate close to pre-existing tissue vasculature, initially growing along such tissue blood vessels, and this phenomenon is important for the metastatic potential which frequently occurs in highly vascularized tissues. Unfortunately, preclinic and clinic anti-angiogenic approaches have not been very successful, and multiple factors have been found to contribute to toxicity and tumor resistance. Moreover, tumors can highlight intrinsic or acquired resistances, or show adaptation to the VEGF-targeted therapies. Furthermore, different mechanisms of vascularization, activation of alternative signaling pathways, and increased tumor aggressiveness make this context even more complex. On the other hand, it has to be considered that the transitional restoration of normal, not fenestrated, microvessels allows the drug to reach the tumor and act with the maximum efficiency. However, these effects are time-limited and different, depending on the various types of cancer, and clearly define a specific “normalization window.” So, new horizons in the therapeutic approaches consist on the treatment of the tumor with pro- (instead of anti-) angiogenic therapies, which could strengthen a network of well-structured blood vessels that facilitate the transport of the drug.
机译:原发性实体瘤起源于预先存在的组织脉管系统,最初沿这种组织血管生长,这种现象对于在高度血管化组织中经常发生的转移潜力很重要。不幸的是,临床前和临床上抗血管生成方法不是很成功,并且发现多种因素可导致毒性和肿瘤抵抗力。此外,肿瘤可以突出内在或获得性耐药性,或显示出对VEGF靶向疗法的适应性。此外,不同的血管形成机制,替代信号通路的激活以及增强的肿瘤侵袭性使这种情况变得更加复杂。另一方面,必须考虑到正常的而非有窗孔的微血管的过渡恢复可以使药物到达肿瘤并发挥最大作用。但是,这些影响是有时间限制的,并且有所不同,具体取决于各种癌症,并且明确定义了特定的“正常化窗口”。因此,治疗方法的新视野在于用促血管生成疗法(而不是抗血管生成疗法)来治疗肿瘤,这可以加强结构良好的血管网络,从而促进药物的运输。

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