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血管内皮生长因子的表达与冠状动脉血管发生和血管生成同时出现。

Vascular endothelial growth factor expression coincides with coronary vasculogenesis and angiogenesis.

作者信息

Tomanek R J, Ratajska A, Kitten G T, Yue X, Sandra A

机构信息

Department of Anatomy and Cell Biology, University of Iowa, Iowa City 52242, USA.

出版信息

Dev Dyn. 1999 May;215(1):54-61. doi: 10.1002/(SICI)1097-0177(199905)215:1<54::AID-DVDY6>3.0.CO;2-0.

Abstract

Vascular endothelial growth factor (VEGF) plays an important role in early embryonic vasculogenesis. To establish its temporal expression and localization in the heart during development, we studied rat hearts from the first embryonic day (E) of myocardial vascular tube formation through the early postnatal period. Ventricular VEGF immunoreactivity was noted in the epicardium and the thin underlying myocardium in E10 ventricles. During the earliest stages of vascularization (E13-E16) immunoreactivity was highest in the compact myocardium nearest the epicardium, and subsequently (E18 and thereafter) became more evenly distributed transmurally. By birth (E22) immunoreactivity was most intense around microvessels. Similarly, VEGF mRNA localization, demonstrated by in situ hybridization, was initially highest near the epicardium and then became more evenly distributed transmurally by late gestation. Within the interventricular septum, the highest expression occurred in the middle of the wall where it correlated with the greatest vascularization. Northern blot analysis showed that from E12 through the first 10 days of postnatal life, VEGF was two to three times higher than in the adult. Western blot analysis showed that VEGF tended to be higher in the atria than the ventricles, and negligible in the outflow tract. Our data indicate that VEGF localization and expression 1) correspond to the pattern of vascularization in the embryonic/fetal heart, and 2) remain high during the early postnatal period when capillary proliferation is high. Because VEGF is stimulated by hypoxia, its preferential mRNA expression near the epicardium, that is, farthest from the ventricular lumen and the O2 source, fits with the hypothesis that a hypoxic gradient is a driving force in the transmural vascularization process.

摘要

血管内皮生长因子(VEGF)在早期胚胎血管生成中起重要作用。为确定其在心脏发育过程中的时间表达及定位,我们研究了从心肌血管管形成的胚胎第1天(E)到出生后早期的大鼠心脏。在E10心室的心室中,VEGF免疫反应性见于心外膜和其下方的薄层心肌。在血管形成的最早阶段(E13 - E16),免疫反应性在最靠近心外膜的致密心肌中最高,随后(E18及以后)在整个心肌壁上分布更均匀。到出生时(E22),微血管周围的免疫反应性最强。同样,原位杂交显示的VEGF mRNA定位最初在靠近心外膜处最高,然后在妊娠后期在整个心肌壁上分布更均匀。在室间隔内,最高表达出现在壁的中部,与最大程度的血管化相关。Northern印迹分析表明,从E12到出生后的前10天,VEGF比成年时高两到三倍。Western印迹分析显示,VEGF在心房中的含量往往高于心室,而在流出道中含量可忽略不计。我们的数据表明,VEGF的定位和表达:1)与胚胎/胎儿心脏的血管化模式相对应;2)在出生后早期毛细血管增殖旺盛时仍保持高水平。由于VEGF受缺氧刺激,其在心外膜附近(即离心室腔和氧气来源最远)的优先mRNA表达符合缺氧梯度是跨壁血管化过程驱动力这一假说。

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