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Expression of an innate immune element (mouse hepcidin-1) in baculovirus expression system and the comparison of its function with synthetic human hepcidin-25

机译:杆状病毒表达系统中先天免疫元件(小鼠hepcidin-1)的表达及其与合成人hepcidin-25的功能比较

摘要

Hepcidin is an innate immune element which decreases the iron absorption from diet and iron releasing from macrophage cell. In contrast to the chemical iron chelators, there has been limited effort applied to the specific use of hepcidin as a new drug for decreasing the iron overload. Hepcidin is produced in different biological systems. For instance, E-coli is used for human hepcidin expression, however, post-translational modification is impaired. We have used a simple baculovirus expression system (BES) to improve the hepcidin folding and activity. Hepcidin Messenger Ribonucleic acid (mRNA) was isolated from mouse liver cells and its complementary Deoxyribonucleic acid (cDNA) was produced and amplified. PFastBac HTB vector was used for recombinant bacmid production. Recombinant baculovirus was produced using SF-9 cell line. The mouse hepcidin-1 protein was expressed in a large quantity and functional tests were performed for this recombinant peptide. The yield of hepcidin in BES was 20 μg/mL and anti-histidine (anti-His) tag antibody was used for the confirmation of hepcidin on western blot nitrocellulose paper. Functional tests showed that mouse hepcidin accumulates iron in the macrophage cell line J774A.1 up to 63%. In addition, our data showed that the mouse hepcidin-1 has less toxicity compared to the synthetic human hepcidin-25 (p = 0.000). © 2011 by School of Pharmacy.
机译:铁调素是一种先天性免疫元件,可减少饮食中铁的吸收和巨噬细胞释放的铁。与化学铁螯合剂相反,对于铁调素作为减少铁超载的新药的特定用途,人们所做的努力有限。铁调素是在不同的生物系统中产生的。例如,大肠杆菌用于人类铁调素的表达,但是翻译后修饰受损。我们已经使用一个简单的杆状病毒表达系统(BES)来改善hepcidin的折叠和活性。从小鼠肝细胞中分离出了Hepcidin Messenger核糖核酸(mRNA),并产生并扩增了其互补的脱氧核糖核酸(cDNA)。 PFastBac HTB载体用于重组杆粒生产。使用SF-9细胞系产生重组杆状病毒。大量表达了小鼠hepcidin-1蛋白,并对该重组肽进行了功能测试。在BES中铁调素的产量为20μg/ mL,抗组氨酸(抗组氨酸)标签抗体用于在免疫印迹硝酸纤维素纸上确认铁调素。功能测试表明,小鼠铁调素在巨噬细胞系J774A.1中积累的铁高达63%。此外,我们的数据显示,与合成的人hepcidin-25相比,小鼠hepcidin-1的毒性较小(p = 0.000)。 ©2011,药学院。

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