Department of Vascular Biology, Graduate School of Dental Medicine, Hokkaido University, Sapporo, Japan.
Cancer Sci. 2013 Nov;104(11):1391-5. doi: 10.1111/cas.12251. Epub 2013 Sep 12.
Tumor blood vessels play important roles in tumor progression and metastasis. Thus, targeting tumor blood vessels is an important strategy for cancer therapy. Tumor endothelial cells (TECs) are the main targets of anti-angiogenic therapy. Although tumor blood vessels generally sprout from pre-existing vessels and have been thought to be genetically normal, they display a markedly abnormal phenotype, including morphological changes. The degree of angiogenesis is determined by the balance between the positive and negative regulating molecules that are released by tumor and host cells in the microenvironment. Reportedly, tumor blood vessels are heterogeneous with TECs differing from normal endothelial cells (in contrast to the conventional view). We recently compared characteristics of different TECs isolated from highly and low metastatic tumors. We found TECs from highly metastatic tumors had more proangiogenic phenotypes than those from low metastatic tumors. Elucidating the variety of TEC phenotypes and identifying TEC molecular signatures should lead to more complete understanding of the mechanisms of tumor progression, discovery of new therapeutic targets, and development of biomarkers. This review considers current studies on TEC heterogeneity and discusses the therapeutic implications of these findings.
肿瘤血管在肿瘤的进展和转移中起着重要的作用。因此,靶向肿瘤血管是癌症治疗的一个重要策略。肿瘤内皮细胞(TEC)是抗血管生成治疗的主要靶点。尽管肿瘤血管通常从预先存在的血管中发芽,并且被认为在遗传上是正常的,但它们表现出明显的异常表型,包括形态变化。血管生成的程度取决于肿瘤和宿主细胞在微环境中释放的正调节和负调节分子之间的平衡。据报道,肿瘤血管是异质的,TEC 与正常内皮细胞不同(与传统观点相反)。我们最近比较了从高转移性和低转移性肿瘤中分离的不同 TEC 的特征。我们发现,高转移性肿瘤的 TEC 比低转移性肿瘤的 TEC 具有更多的促血管生成表型。阐明 TEC 表型的多样性,并确定 TEC 的分子特征,应该能够更全面地了解肿瘤进展的机制,发现新的治疗靶点,并开发生物标志物。这篇综述考虑了目前关于 TEC 异质性的研究,并讨论了这些发现的治疗意义。
