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首页> 外文期刊>Expert opinion on therapeutic targets >Tumour targeting by microtubule-depolymerizing vascular disrupting agents.
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Tumour targeting by microtubule-depolymerizing vascular disrupting agents.

机译:通过微管解聚的血管破坏剂靶向肿瘤。

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摘要

Low molecular weight vascular disrupting agents of the microtubule depolymerizing family cause marked and selective disruption of the established tumour blood vessel network, resulting in tumour cell necrosis. The combretastatins are members of this family and these, together with several other related compounds, have undergone extensive preclinical testing and are now in clinical trials for cancer. Potentially, vascular disrupting agents can also interfere with angiogenesis and constitute a very promising group of novel cancer drugs. In vitro analysis of their signalling activities points to the endothelial cytoskeleton as being their major target and a key player in the events that culminate in vascular collapse. As more of these agents progress into the clinical setting, more research in this area is warranted in order to decipher exact mechanisms responsible for vascular disruption and to understand the reasons for drug selectivity for the tumour vasculature. This information is essential in order to identify new targets within the tumour vasculature and to improve present therapies.
机译:微管解聚家族的低分子量血管破坏剂引起已建立的肿瘤血管网络的明显和选择性破坏,从而导致肿瘤细胞坏死。康普他汀是该家族的成员,并且这些康普他汀与其他几种相关化合物一起接受了广泛的临床前测试,目前正处于癌症的临床试验中。潜在地,血管破坏剂也可能干扰血管生成,并构成非常有希望的新型癌症药物。对其信号传导活性的体外分析指出,内皮细胞骨架是其主要靶点,并且是最终导致血管衰竭的关键因素。随着越来越多的这类药物进入临床,需要在这一领域进行更多的研究,以便破译引起血管破裂的确切机制,并了解对肿瘤脉管系统药物选择性的原因。该信息对于鉴定肿瘤脉管系统内的新靶标并改善现有疗法至关重要。

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