直接检测纤连蛋白的EIIIA和EIIIB可变剪接片段在生理和肿瘤血管生成中的潜在作用。
Direct test of potential roles of EIIIA and EIIIB alternatively spliced segments of fibronectin in physiological and tumor angiogenesis.
作者信息
Astrof Sophie, Crowley Denise, George Elizabeth L, Fukuda Tomohiko, Sekiguchi Kiyotoshi, Hanahan Douglas, Hynes Richard O
机构信息
Howard Hughes Medical Institute, Center for Cancer Research, Department of Biology, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.
出版信息
Mol Cell Biol. 2004 Oct;24(19):8662-70. doi: 10.1128/MCB.24.19.8662-8670.2004.
Abstract
Fibronectin splice variants containing the EIIIA and/or EIIIB exons are prominently expressed in the vasculature of a variety of human tumors but not in normal adult tissues. To understand the functions of these splice variants in physiological and tumor angiogenesis, we used EIIIB-null and EIIIA-null strains of mice to examine neovascularization of mouse retinas, pancreatic tumors in Rip-Tag transgenic mice, and transplanted melanomas. Contrary to expectations, physiological and tumor angiogenesis was not significantly affected by the absence of either EIIIA or EIIIB splice variants. Tumor growth was also not affected. In addition, the expression levels of smooth muscle alpha actin, believed to be modulated by EIIIA-containing fibronectins, were not affected either. Our experiments show that despite their tight regulation during angiogenesis, the presence of EIIIA or EIIIB splice variants individually is not essential for neovascularization.
摘要
含有EIIIA和/或EIIIB外显子的纤连蛋白剪接变体在多种人类肿瘤的脉管系统中显著表达,但在正常成人组织中不表达。为了解这些剪接变体在生理和肿瘤血管生成中的功能,我们使用EIIIB基因敲除和EIIIA基因敲除的小鼠品系来检测小鼠视网膜、Rip-Tag转基因小鼠的胰腺肿瘤以及移植黑色素瘤的新生血管形成。与预期相反,EIIIA或EIIIB剪接变体的缺失并未显著影响生理和肿瘤血管生成。肿瘤生长也未受影响。此外,据信受含EIIIA纤连蛋白调节的平滑肌α肌动蛋白的表达水平也未受影响。我们的实验表明,尽管它们在血管生成过程中受到严格调控,但单独存在EIIIA或EIIIB剪接变体对于新生血管形成并非必不可少。
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