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多种生长因子调节冠状动脉胚胎血管生成。

Multiple growth factors regulate coronary embryonic vasculogenesis.

作者信息

Tomanek R J, Zheng W, Peters K G, Lin P, Holifield J S, Suvarna P R

机构信息

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

出版信息

Dev Dyn. 2001 Jul;221(3):265-73. doi: 10.1002/dvdy.1137.

Abstract

Mechanisms regulating coronary vascularization are not well understood. To test hypotheses regarding the influence of key growth factors and their interactions, we studied vascular tube formation (vasculogenesis) in collagen gels onto which quail embryonic ventricles were placed and incubated in the presence of growth factors or inhibitors. Vasculogenesis in this model is dependent on tyrosine kinase receptors, since tube formation was totally blocked by genestein. Tube formation was attenuated when anti-bFGF or anti-VEGF neutralizing antibodies were added to the medium and nearly completely inhibited when the both were added. The attenuation associated with anti-VEGF was due primarily to a decrease in assembly of endothelial cells, while that associated with bFGF was primarily due to a reduction in endothelial cells. Soluble tie-2, the receptor for angiopoietins, also had an inhibitory effect and, when added with either anti-bFGF or anti-VEGF, markedly attenuated tube formation. At optimal doses, tube formation was enhanced 6.5-fold by bFGF and 2.5-fold by VEGF over the controls. Each of these growth factors was dependent upon the other for optimal induction of tube formation, since neutralizing antibodies to one markedly reduced the potency of the other. VEGF potency was also markedly reduced when soluble tie-2 was added to the medium. Tube formation was virtually totally blocked by exogenous TGF-beta at doses > 1 ng/ml, while neutralizing TGF-beta antibodies enhanced tube formation 2-fold in the 30 ng-30 microg range. These data provide the first documentation of multiple growth factor regulation of coronary tube formation.

摘要

调节冠状动脉血管形成的机制尚未完全明确。为了验证关于关键生长因子的影响及其相互作用的假设,我们研究了鹌鹑胚胎心室置于胶原凝胶上并在生长因子或抑制剂存在下孵育时的血管管形成(血管生成)。该模型中的血管生成依赖于酪氨酸激酶受体,因为染料木黄酮完全阻断了管形成。当向培养基中添加抗bFGF或抗VEGF中和抗体时,管形成减弱,而当两者都添加时,管形成几乎完全被抑制。与抗VEGF相关的减弱主要是由于内皮细胞组装减少,而与bFGF相关的减弱主要是由于内皮细胞减少。血管生成素的受体可溶性tie-2也有抑制作用,当与抗bFGF或抗VEGF一起添加时,显著减弱管形成。在最佳剂量下,与对照组相比,bFGF使管形成增强6.5倍,VEGF使管形成增强2.5倍。这些生长因子中的每一种对于管形成的最佳诱导都依赖于另一种,因为针对一种的中和抗体显著降低了另一种的效力。当向培养基中添加可溶性tie-2时,VEGF的效力也显著降低。当外源性TGF-β剂量>1 ng/ml时,管形成几乎完全被阻断,而在30 ng - 30 μg范围内,中和TGF-β抗体使管形成增强2倍。这些数据首次记录了多种生长因子对冠状动脉管形成的调节作用。

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