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AAV6-mediated Cardiac-specific Overexpression of Ribonucleotide Reductase Enhances Myocardial Contractility.

Mol. Ther.. 2016; 
KolwiczStephen C,OdomGuy L,NowakowskiSarah G,Moussavi-HaramiFarid,ChenXiaolan,ReineckeHans,HauschkaStephen D,MurryCharles E,MahairasGregory G,RegnierMic
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Codon Optimization The final construct was synthesized by Genscript (Piscataway, NJ) and contained the following elements: human cTnT455 RRM1-P2A-RRM2-polyA signal flanked by NotI sites...Human RRM1 (NM_001033.3) and RRM2 (NM_001034) sequences were codon optimized for expression in human using Genscript's OptimumGene Codon Optimization Analysis (includes analysis of codon usage bias, GC content, CpG dinucleotide content, mRNA secondary structure, cryptic splicing sites, premature polyA sites, internal chi sites and ribosomal binding sites, negative CpG islands, RNA instability motifs, repeat sequences, and restriction sites that may interfere with cloning). Get A Quote

摘要

Impaired systolic function, resulting from acute injury or congenital defects, leads to cardiac complications and heart failure. Current therapies slow disease progression but do not rescue cardiac function. We previously reported that elevating the cellular 2 deoxy-ATP (dATP) pool in transgenic mice via increased expression of ribonucleotide reductase (RNR), the enzyme that catalyzes deoxy-nucleotide production, increases myosin-actin interaction and enhances cardiac muscle contractility. For the current studies, we initially injected wild-type mice retro-orbitally with a mixture of adeno-associated virus serotype-6 (rAAV6) containing a miniaturized cardiac-specific regulatory cassette (cTnT(455)) co... More

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