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首页> 外文期刊>BioMetals: An International Journal on the Role of Metal Ions in Biology, Biochemistry and Medicine >Human apo-lactoferrin as a physiological mimetic of hypoxia stabilizes hypoxia-inducible factor-1 alpha
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Human apo-lactoferrin as a physiological mimetic of hypoxia stabilizes hypoxia-inducible factor-1 alpha

机译:人脱辅乳铁蛋白作为低氧的生理模拟物可稳定低氧诱导因子-1α

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摘要

Apo-form of human lactoferrin (LF) is a potent iron chelator, this feature being similar to the iron-binding properties of a synthetic chelator desferoxamine (DFO). The latter stabilizes the principal adaptive transcriptional hypoxia-inducible factor-1 alpha (HIF-1a). Since DFO is known as a pharmacological mimetic of hypoxia it was decided to test whether apo-LF is able to perform as such. Mice either injected intraperitoneally or given per os apo-LF displayed HIF-1a in liver, lungs, heart, brain, spleen and kidneys, as judged by results of Western blotting. Similar administration of iron-saturated LF (75 mg/kg) did not bring forth such effect. Synthesis of erythropoietin and ceruloplasmin became increased in the first case, which is explained by the respective genes being targets for HIF-1a. Apo-LF, but not Fe-LF, injected intraperitoneally to hypoxia low-resistant mice 24 h before animals were subjected to normobaric hypoxia with hypercapnia caused a significant increase of life-time by 40 %. The results obtained show that, like DFO, apo-LF performs as a normoxic mimetic of hypoxia, capable of stabilizing HIF-1a. Protective features of LF and DFO and their pharmacological properties involving HIF-1a are discussed.
机译:人乳铁蛋白(LF)的脱辅基形式是有效的铁螯合剂,此功能类似于合成螯合剂去铁胺(DFO)的铁结合特性。后者稳定了主要的适应性转录缺氧诱导因子1α(HIF-1a)。由于DFO被称为低氧的药理模拟物,因此决定测试apo-LF是否能够如此发挥作用。通过Western印迹的结果判断,经腹膜内注射或经口服apo-LF给予的小鼠在肝,肺,心脏,脑,脾脏和肾脏中显示出HIF-1a。铁饱和LF(75 mg / kg)的类似给药没有产生这种效果。在第一种情况下,促红细胞生成素和铜蓝蛋白的合成增加,这可以通过将各自的基因作为HIF-1a的靶标来解释。在动物经历常压低氧合并高碳酸血症之前24小时,将Apo-LF而非Fe-LF腹膜内注射至低氧低抗性小鼠,导致寿命显着增加40%。获得的结果表明,与DFO一样,apo-LF可以作为缺氧的常氧模拟物,能够稳定HIF-1a。讨论了LF和DFO的保护特性及其涉及HIF-1a的药理特性。

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