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Vascular contribution to metastasis

机译:血管对转移的贡献

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It has been 40 years since Folkman’s seminal paper [Cancer Res 1974. 34:2109-13], proposing the presence of a tumour associated angiogenic factor, which could be targeted as an anticancer therapy. There are currently a handful of drugs in trial or use that have been marketed as targeting angiogenesis. Unfortunately, the most widely used of these, bevacizumab (Avastin?, Roche), has met with limited success clinically. For this reason and based on a calculation of cost benefit, bevacizumab is now only publically subsidised for use in a limited range of solid tumours. That the contribution of vasculature to malignancy remains poorly understood is increasingly clear. At the same time, the traditional view that vascularisation is a passive participant in the process of malignancy, and that endothelium merely provides a conduit by which tumour cells spread, is being replaced with an understanding that vasculature is a key player in the process of metastasis. Furthermore, the identification of non-traditional sources of vasculature has complicated our understanding of the tumour endothelium as a unique population that can be simply targeted as an anticancer therapy. The following review seeks to provide an up-to-date view of vascular contribution to metastasis and implications for new vasculature-targeted anticancer treatments.
机译:自Folkman的开创性论文[Cancer Res 1974. 34:2109-13]提出以来已有40年,该研究提出存在与肿瘤相关的血管生成因子,该因子可作为抗癌治疗的目标。目前,有少数药物正在试验或使用中,以靶向血管生成的形式销售。不幸的是,其中最广泛使用的贝伐单抗(Avastin ?,罗氏公司)在临床上取得了有限的成功。因此,基于成本收益的计算,贝伐单抗目前仅在有限的实体瘤范围内得到公共补贴。脉管系统对恶性肿瘤的作用仍然知之甚少,这一点越来越清楚。同时,传统的观点认为血管化是恶性肿瘤过程的被动参与者,而内皮仅提供肿瘤细胞扩散的管道,这种观点被脉管系统在转移过程中起关键作用的理解所取代。 。此外,对非传统脉管系统来源的鉴定使我们对肿瘤内皮作为一个独特的人群的理解变得复杂,该人群可以简单地作为抗癌治疗的目标。以下综述旨在提供有关血管对转移的贡献及其对靶向新血管系统的抗癌治疗的影响的最新观点。

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