Cre and GFP expressing (RGD fiber modified) Adenovirus
The cell entry of adenovirus is dependent on the initial recognition of the coxsackie-adenovirus receptor (CAR) on the surafce, therefore the infection efficiency of adenovirus is very low for cells with low or no CAR receptor. An Arg-Gly-Asp (RGD) motif was introduced in the surface-exposed loop of the adenovirus fiber knob, this enables the adenovirus to bypass CAR and mediate cell entry via RGD binding integrins.
RDG modified adenovirus can be used for “retargeting” cells that regular adenovirus doesn’t work well. The infection effeciency of RDG modified adenovirus can be tens or hundreds of times higher than standard Ad5 in some cells, including human or mouse macrophages and T cells etc.
This is a RGD modified replication-deficient adenovirus expressing codon optimized Cre and GFP under a CMV promoter. The Cre and GFP are separated by a 2A peptide.
Ready-to-use Cre and GFP expressing (RGD fiber modified) Adenovirus. Ad(RGD)-GFP-2A-iCre 1779 GFP Cre RDG adenovirus
Related Citations
- ETV7 is an essential component of a rapamycin-insensitive mTOR complex in cancer. FC Harwood,etc, (2018), Science Advances,
- Genome Modification Leads to Phenotype Reversal in Human Myotonic Dystrophy type 1 iPS-cell Derived Neural Stem Cells. G Xia, etc, (2015), STEM CELLS
- Fine-Tuning of the RIG-I-Like Receptor/Interferon Regulatory Factor 3-Dependent Antiviral Innate Immune Response by the Glycogen Synthase Kinase 3/ß-Catenin Pathway. KA Khan, etc, (2015), Molecular and Cellular Biology