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转录因子PEBP2/CBF在小鼠内皮细胞MSS31血管生成活性中的不可或缺作用。

Indispensable role of the transcription factor PEBP2/CBF in angiogenic activity of a murine endothelial cell MSS31.

作者信息

Namba K, Abe M, Saito S, Satake M, Ohmoto T, Watanabe T, Sato Y

机构信息

Department of Vascular Biology, Institute of Development, Aging and Cancer, Tohoku University, 4-1 Seiryo-machi, Aoba-ku, Sendai 980-8575, Japan.

出版信息

Oncogene. 2000 Jan 6;19(1):106-14. doi: 10.1038/sj.onc.1203257.

DOI:10.1038/sj.onc.1203257
PMID:10644985
Abstract

Mice lacking the AML1/PEBP2alphaB/CBFa2 gene or PEBP2beta/CBFb gene exhibit a defect in definitive hematopoiesis and die in utero because of hemorrhage in the central nervous system. Hematopoiesis in the embryo is considered to be tightly associated with vascular development. Here we examined whether PEBP2/CBF plays any role in angiogenesis besides that in definitive hematopoiesis. We found that AML1/PEBP2alphaB/CBFa2, PEBP2alphaA/CBFa1, and PEBP2beta/CBFb were expressed in a murine endothelial cell line MSS31. The expression of these molecules as well as the DNA binding activity of PEBP2/CBF were augmented by angiogenic growth factors such as bFGF and VEGF. Moreover, the expression of PEBP2 alpha/CBFa protein in endothelial cells was confirmed at the site of angiogenesis in vivo. To further clarify the role of PEBP2/CBF in angiogenesis, we established permanent transfectants of PEBP2 beta-MYH11 gene, one that interacts with the runt domain of the alpha subunit and deregulates PEBP2/CBF in a dominant interfering manner. Proliferation, migration, and tube formation of the PEBP2 beta-MYH11 transfectants were significantly reduced in comparison with those activities of the mock transfectants. These results suggest that transcription factor PEBP2/CBF plays an important role in angiogenesis.

摘要

缺乏AML1/PEBP2alphaB/CBFa2基因或PEBP2beta/CBFb基因的小鼠在确定性造血过程中存在缺陷,并因中枢神经系统出血而在子宫内死亡。胚胎中的造血作用被认为与血管发育紧密相关。在此,我们研究了PEBP2/CBF除了在确定性造血过程中之外,是否在血管生成中发挥任何作用。我们发现AML1/PEBP2alphaB/CBFa2、PEBP2alphaA/CBFa1和PEBP2beta/CBFb在小鼠内皮细胞系MSS31中表达。这些分子的表达以及PEBP2/CBF的DNA结合活性被血管生成生长因子如bFGF和VEGF增强。此外,在内皮细胞中PEBP2 alpha/CBFa蛋白的表达在体内血管生成部位得到证实。为了进一步阐明PEBP2/CBF在血管生成中的作用,我们构建了PEBP2 beta-MYH11基因的永久转染细胞系,该基因与α亚基的 runt 结构域相互作用,并以显性干扰方式使PEBP2/CBF失调。与空载体转染细胞系相比,PEBP2 beta-MYH11转染细胞系的增殖、迁移和管形成能力显著降低。这些结果表明转录因子PEBP2/CBF在血管生成中起重要作用。

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