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Effects of Self-Complementarity Codon Optimization Transgene and Dose on Liver Transduction with AAV8

机译:自我互补密码子优化转基因和剂量对AAV8肝转导的影响

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摘要

Numerous methods of vector design and delivery have been employed in an attempt to increase transgene expression following AAV-based gene therapy. Here, a gene transfer study was conducted in mice to compare the effects of vector self-complementarity (double- or single-stranded DNA), codon optimization of the transgene, and vector dose on transgene expression levels in the liver. Two different reporter genes were used: human ornithine transcarbamylase (hOTC) detected by immunofluorescence, and enhanced green fluorescent protein (EGFP) detected by direct fluorescence. The AAV8 capsid was chosen for all experiments due to its strong liver tropism. While EGFP is already a codon-optimized version of the original gene, both wild-type (WT) and codon-optimized (co) versions of the hOTC transgene were compared in this study. In addition, the study evaluated which of the two hOTC modifications—codon optimization or self-complementarity—would confer the highest increase in expression levels at a given dose. Interestingly, based on morphometric image analysis, it was observed that the difference in detectable expression levels between self-complementary (sc) and single-stranded (ss) hOTCco vectors was dose dependent, with a sevenfold increase in OTC-positive area using sc vectors at a dose of 3 × 109 genome copies (GC) per mouse, but no significant difference at a dose of 1 × 1010 GC/mouse. In contrast, with EGFP as a transgene, the increases in expression levels when using the sc vector were observed at both the 3 × 109 GC/mouse and 1 × 1010 GC/mouse doses. Furthermore, codon optimization of the hOTC transgene generated a more significant improvement in expression than the use of self-complementarity did. Overall, the results demonstrate that increases in expression levels gained by using sc vectors instead of ss vectors can vary between different transgenes, and that codon optimization of the transgene can have an even more powerful effect on the resulting expression levels.
机译:已经尝试了多种载体设计和递送方法,以尝试在基于AAV的基因治疗后增加转基因表达。此处,在小鼠中进行了基因转移研究,以比较载体自身互补性(双链或单链DNA),转基因密码子优化以及载体剂量对肝脏中转基因表达水平的影响。使用了两种不同的报告基因:通过免疫荧光检测的人鸟氨酸转氨甲酰酶(hOTC)和通过直接荧光检测的增强型绿色荧光蛋白(EGFP)。由于AAV8衣壳具有强烈的肝向性,因此被选择用于所有实验。尽管EGFP已经是原始基因的密码子优化版本,但在本研究中比较了hOTC转基因的野生型(WT)和密码子优化(co)版本。此外,该研究评估了在给定剂量下,两种hOTC修饰中的哪一个(密码子优化或自我互补)会带来最高的表达水平增加。有趣的是,基于形态图像分析,观察到自我互补(sc)和单链(ss)hOTCco载体之间可检测的表达水平差异是剂量依赖性的,使用sc载体的OTC阳性面积增加了7倍每只小鼠的3×10 9 基因组拷贝(GC)剂量,但每只小鼠1×10 10 GC剂量下无显着差异。相比之下,以EGFP作为转基因,使用sc载体时,在3×10 9 GC /小鼠和1×10 10 处均观察到表达水平的增加。 GC /小鼠剂量。此外,与使用自互补性相比,hOTC转基因的密码子优化在表达上产生了更显着的改善。总体而言,结果表明,通过使用sc载体而不是ss载体获得的表达水平的提高在不同的转基因之间会有所不同,并且转基因的密码子优化可能对所得表达水平产生更强大的影响。

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