首页> 外文期刊>American Journal of Physiology >VEGF causes pulmonary hemorrhage, hemosiderosis, and air space enlargement in neonatal mice.
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VEGF causes pulmonary hemorrhage, hemosiderosis, and air space enlargement in neonatal mice.

机译:VEGF在新生小鼠中引起肺出血,含铁血黄素沉着和气隙增大。

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摘要

To determine whether increased levels of VEGF disrupt postnatal lung formation or function, conditional transgenic mice in which VEGF 164 expression was enhanced in respiratory epithelial cells were produced. VEGF expression was induced in the lungs of VEGF transgenic pups with doxycycline from postnatal day 1 through 2 and 6 wk of age. VEGF levels were higher in bronchoalveolar lavage fluid (BALF) and lung homogenates of VEGF transgenic mice compared with endogenous VEGF levels in controls. Neonatal mortality was increased by 50% in VEGF transgenic mice. Total protein content in BALF was elevated in VEGF transgenic mice. Surfactant protein B protein expression was unaltered in VEGF transgenic mice. Although postnatal alveolar and vascular development were not disrupted by VEGF expression, VEGF transgenic mice developed pulmonary hemorrhage, alveolar remodeling, and macrophage accumulation as early as 2 wk of age. Electron microscopy demonstrated abnormal alveolar capillary endothelium in the VEGF transgenic mice. In many locations, the endothelium was discontinuous with segments of attenuated endothelial cells. Large numbers of hemosiderin-laden macrophages and varying degrees of emphysema were observed in adult VEGF transgenic mice. Overexpression of VEGF in the neonatal lung increased infant mortality and caused pulmonary hemorrhage, hemosiderosis, alveolar remodeling, and inflammation.
机译:为了确定增加的VEGF水平是否破坏了出生后肺的形成或功能,产生了其中呼吸道上皮细胞中VEGF 164表达增强的条件性转基因小鼠。从出生后第1天,第2天和第6周龄开始,用强力霉素在VEGF转基因幼崽的肺中诱导VEGF表达。与对照组中的内源性VEGF水平相比,在VEGF转基因小鼠的支气管肺泡灌洗液(BALF)和肺匀浆中,VEGF水平更高。 VEGF转基因小鼠的新生儿死亡率提高了50%。在VEGF转基因小鼠中BALF中的总蛋白质含量升高。在VEGF转基因小鼠中表面活性剂蛋白B蛋白表达未改变。尽管出生后的肺泡和血管发育不受VEGF表达的干扰,但VEGF转基因小鼠早在2周龄时就出现了肺出血,肺泡重塑和巨噬细胞蓄积。电子显微镜显示在VEGF转基因小鼠中肺泡毛细血管内皮细胞异常。在许多位置,内皮是不连续的,具有减薄的内皮细胞片段。在成年VEGF转基因小鼠中观察到大量含铁血黄素的巨噬细胞和不同程度的肺气肿。新生儿肺中VEGF的过度表达会增加婴儿死亡率,并引起肺出血,含铁血黄素沉着症,肺泡重塑和炎症。

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