可溶性EphB4对肿瘤生长和血管生成的抑制作用。

Georg Martiny-Baron, Thomas Korff, Florence Schaffner, Norbert Esser, Stefan Eggstein, Dieter Marmé, Hellmut G Augustin
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引用次数: 0

摘要

EphB受体及其ephrinB配体在正常血管系统的形成中起着关键作用。最近的研究也表明Eph/ephrin相互作用参与恶性肿瘤的进展和血管生成。我们制备了表达A375黑色素瘤细胞的可溶性单体EphB4 (sEphB4),以研究显性负作用的sEphB4对肿瘤生长和血管生成的影响。与对照肿瘤相比,裸鼠皮下生长的可溶性ephb4表达的A375肿瘤的生长显著降低。表达sephb4的细胞在单层培养中的增殖能力没有改变。然而,表达sephb4的A375细胞不能在三维球体中建立适当的细胞-细胞接触。然而,在体外三维培养或体内皮下肿瘤中,sEphB4转染物的增殖和凋亡率降低。肿瘤的血管表型分析显示,在表达sephb4的肿瘤中,肿瘤内微血管密度降低。与这些小鼠实验相对应,对人结肠癌中EphB4和ephrinB2表达的配对分析显示,与邻近正常组织相比,EphB4的表达水平显著上调。综上所述,这些数据确定了sEphB4对肿瘤和血管室的双重作用,共同抑制肿瘤生长。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Inhibition of tumor growth and angiogenesis by soluble EphB4.

EphB receptors and their ephrinB ligands play a key role in the formation of a regular vascular system. Recent studies have also shown the involvement of Eph/ephrin interactions in malignant tumor progression and angiogenesis. We have generated soluble monomeric EphB4 (sEphB4)-expressing A375 melanoma cells to study the effect of dominant negatively acting sEphB4 on tumor growth and angiogenesis. Soluble EphB4-expressing A375 tumors grown subcutaneously in nude mice show dramatically reduced tumor growth compared to control tumors. The proliferative capacity of sEphB4-expressing cells in monolayer culture is not altered. Yet, sEphB4-expressing A375 cells cannot establish proper cell-cell contacts in three-dimensional spheroids. However, sEphB4 transfectants have reduced proliferation and apoptosis rates when grown in three-dimensional culture in vitro or in subcutaneous tumors in vivo. Analysis of the vascular phenotype of the tumors revealed a reduction of intratumoral microvessel density in sEphB4-expressing tumors. Corresponding to these mouse experiments, a matched pair analysis of EphB4 and ephrinB2 expression in human colon carcinomas revealed significantly upregulated levels of EphB4 expression compared to adjacent normal tissue. Taken together, the data identify dual effects of sEphB4 on the tumor and the vascular compartment that collectively inhibit tumor growth.

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