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首页> 外文期刊>Hypertension: An Official Journal of the American Heart Association >Transduction of a Functional Domain of the AT1 Receptor in Neurons by HIV-Tat PTD
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Transduction of a Functional Domain of the AT1 Receptor in Neurons by HIV-Tat PTD

机译:HIV-Tat PTD对神经元中AT1受体功能域的转导

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Despite advances in transgenic and gene transfer technologies, in vivo structure–function studies of the angiotensin II type I receptor (AT1R) have revealed limited information on the diverse actions of angiotensin II. Our objective in the present study was to determine if protein transduction technology with the use of the HIV-Tat protein transduction domain could fill this gap. Recombinant HIV-Tat protein transduction domain fused to EGFP and to the third intracellular loop of the AT1R was expressed. Incubation of hypothalamus and brainstem neurons with this peptide indicated an efficient transport of the protein to most of the cells. This transduction was accompanied by an increase in neuronal firing rate, an effect similar to that observed with angiotensin II stimulation of the neuronal AT1R. The characteristics of the chronotropic effects of recombinant third intracellular loop and its synthetic counterpart were similar and comparable to the effects of angiotensin II on these neurons. In addition, in the presence of the protein kinase C inhibitor calphostin C, the peptide failed to increase firing rate. These observations demonstrated that transduction of neurons with the third intracellular loop of the AT1R produces chronotropic effects similar to those induced by angiotensin II. The data suggests that protein transduction technology could be useful for in vivo AT1R domain transduction.
机译:尽管转基因和基因转移技术取得了进步,但对血管紧张素II型I受体(AT1R)的体内结构功能研究表明,有关血管紧张素II的多种作用的信息有限。我们在本研究中的目的是确定使用HIV-Tat蛋白转导结构域的蛋白转导技术是否可以填补这一空白。表达了与EGFP和AT1R的第三个细胞内环融合的重组HIV-Tat蛋白转导结构域。下丘脑和脑干神经元与该肽的温育表明该蛋白有效运输到大多数细胞。这种转导伴随着神经元放电速率的增加,类似于血管紧张素II刺激神经元AT1R所观察到的效果。重组第三胞内环及其合成对应物的变时作用的特征与血管紧张素II对这些神经元的作用相似且相当。另外,在蛋白激酶C抑制剂钙磷蛋白C的存在下,该肽不能提高射击速率。这些观察结果表明,利用AT1R的第三个细胞内环转导神经元会产生与血管紧张素II相似的变时性作用。数据表明蛋白质转导技术可用于体内AT1R结构域转导。

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