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肿瘤血管生成:病理生理学与临床意义

Tumour angiogenesis: pathophysiology and clinical significance.

作者信息

Lichtenbeld H H, van Dam-Mieras M C, Hillen H F

机构信息

Department of Internal Medicine, University Hospital Maastricht, Netherlands.

出版信息

Neth J Med. 1996 Jul;49(1):42-51. doi: 10.1016/0300-2977(95)00117-4.

Abstract

In the 1970s it was first proposed that tumours depended on the establishment of a microcirculation in order to grow beyond a few millimetres. Thereafter, the search to prove this hypothesis increased strongly and by the end of the 1980s, evidence was given that tumours were angiogenesis-dependent and metastatic cells were only shed after the tumour had established its microcirculation. The process of neovascularization is regulated by numerous growth factors, vascular endothelial cells, and matrix proteins released from host stromal cells such as macrophages and mast cells. The process of tumour growth and metastasis involves tumour cell-host cell and cell-matrix interactions and many of the underlying mechanisms of these interactions still remain to be elucidated. Although in a minority of cases treatment of solid tumours has been effectively improved, for the majority of cases more adequate treatment is still required to reduce the mortality rate. It has been proposed only recently that specific targeting of the angiogenic process might inhibit tumour growth and metastasis. This promising field of research is now exponentially growing. It is the purpose of this review to summarize current knowledge on the pathophysiology and clinical significance of tumour angiogenesis.

摘要

20世纪70年代首次提出,肿瘤要生长到几毫米以上就必须建立微循环。此后,为证明这一假说的研究力度大幅增强,到20世纪80年代末,有证据表明肿瘤依赖血管生成,转移细胞只有在肿瘤建立微循环后才会脱落。新生血管形成过程受多种生长因子、血管内皮细胞以及宿主基质细胞(如巨噬细胞和肥大细胞)释放的基质蛋白调控。肿瘤生长和转移过程涉及肿瘤细胞与宿主细胞以及细胞与基质的相互作用,而这些相互作用的许多潜在机制仍有待阐明。尽管在少数情况下实体瘤的治疗已得到有效改善,但对于大多数病例,仍需要更充分的治疗以降低死亡率。直到最近才有人提出,特异性靶向血管生成过程可能抑制肿瘤生长和转移。这个充满前景的研究领域目前正呈指数级增长。本综述的目的是总结目前关于肿瘤血管生成的病理生理学和临床意义的知识。

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