HGF Airway Over-expression Leads to Enhanced Pulmonary Vascularization without Induction of VEGF.

Current angiogenesis Pub Date : 2012-02-01 Epub Date: 2012-03-28 DOI:10.2174/2211552811201010052
Cassandra Henry, Ariel Lopez-Chavez, Laura P Stabile, Jill M Siegfried
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引用次数: 1

Abstract

The hepatocyte growth factor (HGF)/c-Met signaling pathway mediates angiogenesis. We have previously reported that airway expression of a human HGF transgene (HGF TG) produced mice that were more susceptible to lung tumorigenesis induced by 4-(methylnitrosoamino)-1-(3-pyridyl)-1-butanone (NNK). Here we show untreated HGF TG mice display enhanced vascularization (40 wks) and enhanced lymph vessel formation (20 wks) in the lungs compared to wild-type (WT) littermates, as ascertained by microvessel density. We profiled mRNA expression from HGF TG and WT mice for genes involved in angiogenesis. We consistently found significant decreases in expression of the VEGF family of angiogenic genes, including Vegfa, Vegfb, Vegfc, and Vegfd / Figf. Decreases were confirmed in whole lung protein extracts by immunoblot. Similar patterns of down-regulation were observed at 10, 20, and 40 wks of age. Vandetanib, an inhibitor of VEGFR2 and VEGFR3, did not prevent the increase in microvessel density observed in HGF TG mice. Reduction in VEGF pathway genes was also detected in lung tumors derived from NNK-treated HGF TG mice. HGF TG lung tumors also showed increased expression of five Cxcl family genes including Cxcl1 and Cxcl2 (murine forms of IL8). These results suggest increased vascularization produced by airway over-expression of HGF occurs through direct activation of c-Met on endothelial cells, rather than induction of VEGF pathways. Elevated HGF may also increase expression of inflammatory mediators that contribute to lung tumor progression.

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HGF气道过表达导致肺血管化增强而不诱导VEGF。
肝细胞生长因子(HGF)/c-Met信号通路介导血管生成。我们之前报道过,气道表达人HGF转基因(HGF TG)使小鼠更容易受到4-(甲基亚硝基氨基)-1-(3-吡基)-1-丁酮(NNK)诱导的肺肿瘤发生。本研究显示,与野生型(WT)幼崽相比,未经治疗的HGF TG小鼠肺部血管化(40周)和淋巴管形成(20周)增强,这是通过微血管密度确定的。我们分析了HGF、TG和WT小鼠血管生成相关基因的mRNA表达。我们一致发现血管生成基因VEGF家族的表达显著降低,包括Vegfa、Vegfb、Vegfc和Vegfd / Figf。免疫印迹法证实全肺蛋白提取物减少。在10、20和40周龄时观察到类似的下调模式。Vandetanib, VEGFR2和VEGFR3的抑制剂,不能阻止HGF TG小鼠微血管密度的增加。在nnk处理的HGF TG小鼠的肺肿瘤中也检测到VEGF通路基因的减少。HGF - TG肺肿瘤也显示5个Cxcl家族基因的表达增加,包括Cxcl1和Cxcl2(小鼠形式的IL8)。这些结果表明,气道过度表达HGF产生的血管化增加是通过直接激活内皮细胞上的c-Met,而不是诱导VEGF通路发生的。升高的HGF也可能增加促进肺肿瘤进展的炎症介质的表达。
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