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多步骤肿瘤进展过程中内皮祖细胞的血管整合

Vascular integration of endothelial progenitors during multistep tumor progression.

作者信息

Hämmerling Günter J, Ganss Ruth

机构信息

Department of Molecular Immunology, German Cancer Research Center, Heidelberg, Germany.

出版信息

Cell Cycle. 2006 Mar;5(5):509-11. doi: 10.4161/cc.5.5.2517. Epub 2006 Mar 1.

Abstract

Bone marrow-derived endothelial precursor cells contribute to tumor neovascularization. However, it is unclear when during progressive tumor growth circulating precursors are recruited into the preexisting vascular network, and how they home specifically into the tumor microenvironment. Here, we summarize recent findings from mouse models of multistage carcinogenesis, which reveal distinct phases of angiogenic activity. Only advanced tumors with a highly heterogeneous, sprouting vasculature recruite endothelial progenitors into neovessels. Surprisingly, during progressive tumor growth endothelial cells acquire new characteristics and secrete CC chemokines, a group of chemoattractants with adjacent cysteins, which play a dual role by enhancing neovascularization in an autocrine and endocrine fashion. Locally, chemokines stimulate endothelial proliferation; systemically, they guide chemokine receptor-positive circulating progenitors into the tumor bed. Subsequently, endothelial progenitors are truly integrated into the network of pre-existing vessels. This mechanism represents a novel concept where not the tumor itself, but endothelial cells as components of the tumor-induced stroma foster neovascularization in a self-amplifying loop.

摘要

骨髓来源的内皮祖细胞有助于肿瘤新生血管形成。然而,在肿瘤进行性生长过程中,循环祖细胞何时被招募到已有的血管网络中,以及它们如何特异性归巢到肿瘤微环境中尚不清楚。在此,我们总结了多阶段致癌小鼠模型的最新研究结果,这些结果揭示了血管生成活性的不同阶段。只有具有高度异质性、发芽状血管的晚期肿瘤才会将内皮祖细胞招募到新生血管中。令人惊讶的是,在肿瘤进行性生长过程中,内皮细胞获得了新的特性并分泌CC趋化因子,这是一组具有相邻半胱氨酸的化学引诱剂,它们通过自分泌和内分泌方式增强新生血管形成,发挥双重作用。在局部,趋化因子刺激内皮细胞增殖;在全身,它们引导趋化因子受体阳性的循环祖细胞进入肿瘤床。随后,内皮祖细胞真正整合到已有的血管网络中。这种机制代表了一种新的概念,即不是肿瘤本身,而是作为肿瘤诱导基质成分的内皮细胞以自我放大的循环促进新生血管形成。

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