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Effects of self-complementarity, codon optimization, transgene, and dose on liver transduction with AAV8.

Hum Gene Ther Methods.. 2016-12;  27(6):228-237
Bell Peter, Wang Lili, Chen Shu-Jen, Yu Hongwei, Zhu Yanqing, Nayal Mohamad, He Zhenning, White John, Lebel-Hagan Deborah, and Wilson James M. Gene Therapy Program, Department of Medicine, University of Pennsylvania, 125 S. 31st Street, TRL 2000, Philadelphia, PA 19104.
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Abstract

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 ge... More

Keywords

AAV8; codon optimization; liver gene transfer; self-complementarity