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首页> 外文期刊>Biochemical and Biophysical Research Communications >A site-specific genomic integration strategy for sustained expression of glucagon-like peptide-1 in mouse muscle for controlling energy homeostasis.
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A site-specific genomic integration strategy for sustained expression of glucagon-like peptide-1 in mouse muscle for controlling energy homeostasis.

机译:一种特定位点的基因组整合策略,可在小鼠肌肉中持续表达胰高血糖素样肽1,以控制能量稳态。

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摘要

The incretin hormone glucagon-like peptide-1 (GLP-1) exerts important functions in controlling glucose and energy homeostasis. Endogenous GLP-1 has a very short half-life due to DPP-IV-mediated degradation and renal clearance, which limits the therapeutic use of native GLP-1. We have shown previously that immunoglobulin fragment-fused GLP-1 (GLP-1/Fc) is a structurally stable GLP-1 analog. Here, we report a non-viral GLP-1/Fc gene therapy strategy utilizing a REP78-in-trans and REB-in-cis element system to achieve a site-specific genomic integration. For this purpose, the GLP-1/Fc expression cassette, which is fused with the RBE element, was co-injected with the Rep78 plasmid into the muscles of transgenic mice carrying the AAVS1 locus of human chromosome 19. The Rep protein-mediated site-specific integration was demonstrated by nested PCR, dot-blot, and Southern blotting. We found that this approach reduced weight gain and improved lipid profiles in the AAVS1-mice on high-fat diet challenge. Our observations reveal a new GLP-1 therapeutic strategy with an apparent absence of side effects, which may find applications in diabetes treatment and obesity prevention.
机译:肠降血糖素激素胰高血糖素样肽1(GLP-1)在控制葡萄糖和能量稳态方面发挥重要作用。内源性GLP-1由于DPP-IV介导的降解和肾脏清除而具有非常短的半衰期,这限制了天然GLP-1的治疗用途。先前我们已经证明,免疫球蛋白片段融合的GLP-1(GLP-1 / Fc)是结构稳定的GLP-1类似物。在这里,我们报告了一种非病毒GLP-1 / Fc基因治疗策略,利用REP78-in-trans和REB-in-cis元件系统来实现位点特异性基因组整合。为此,将与RBE元件融合的GLP-1 / Fc表达盒与Rep78质粒共注射到携带人19号染色体AAVS1基因座的转基因小鼠的肌肉中。Rep蛋白介导的位点巢式PCR,斑点印迹和Southern印迹证实了特异性整合。我们发现,这种方法降低了高脂饮食对AAVS1-小鼠体重的增加并改善了其脂质分布。我们的观察结果揭示了一种新的GLP-1治疗策略,显然没有副作用,这可能在糖尿病治疗和肥胖症预防中得到应用。

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