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The vascular endothelial growth factor (VEGF) isoforms: differential deposition into the subepithelial extracellular matrix and bioactivity of extracellular matrix-bound VEGF.

机译:血管内皮生长因子(VEGF)亚型:差异沉积到上皮下细胞外基质中以及与细胞外基质结合的VEGF的生物活性。

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摘要

Vascular endothelial growth factor (VEGF)mRNA undergoes alternative splicing events that generate four different homodimeric isoforms, VEGF121, VEGF165, VEGF189, or VEGF206. VEGF121 is a nonheparin-binding acidic protein, which is freely diffusible. The longer forms, VEGF189 or VEGF206, are highly basic proteins tightly bound to extracellular heparin-containing proteoglycans. VEGF165 has intermediate properties. To determine the localization of VEGF isoforms, transfected human embryonic kidney CEN4 cells expressing VEGF165, VEGF189, or VEGF206 were stained by immunofluorescence with a specific monoclonal antibody. The staining was found in patches and streaks suggestive of extracellular matrix (ECM). VEGF165 was observed largely in Golgi apparatus-like structures. Immunogold labeling of cells expressing VEGF189 or VEGF206 revealed that the staining was localized to the subepithelial ECM. VEGF associated with the ECM was bioactive, because endothelial cells cultured on ECM derived from cells expressing VEGF189 or VEGF206 were markedly stimulated to proliferate. In addition, ECM-bound VEGF can be released into a soluble and bioactive form by heparin or plasmin. ECM-bound VEGF189 and VEGF206 have molecular masses consistent with the intact polypeptides. The ECM may represent an important source of VEGF and angiogenic potential.
机译:血管内皮生长因子(VEGF)mRNA经历了其他剪接事件,产生了四种不同的同型二聚体同型物,即VEGF121,VEGF165,VEGF189或VEGF206。 VEGF121是非肝素结合性酸性蛋白,可自由扩散。较长的形式是VEGF189或VEGF206,是高度碱性的蛋白质,与含细胞外肝素的蛋白聚糖紧密结合。 VEGF165具有中间性质。为了确定VEGF同工型的定位,用特异性单克隆抗体通过免疫荧光对表达VEGF165,VEGF189或VEGF206的转染的人胚肾CEN4细胞进行染色。在表明细胞外基质(ECM)的斑块和条纹中发现了染色。在高尔基体装置样结构中主要观察到VEGF165。表达VEGF189或VEGF206的细胞的免疫金标记显示染色位于局部上皮下ECM。与ECM相关的VEGF具有生物活性,因为在ECM上培养的内皮细胞可显着刺激其增殖,这些内皮细胞来自表达VEGF189或VEGF206的细胞。此外,ECM结合的VEGF可以通过肝素或纤溶酶释放为可溶的生物活性形式。与ECM结合的VEGF189和VEGF206具有与完整多肽一致的分子量。 ECM可能代表VEGF和血管生成潜力的重要来源。

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