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Publication : Development of an inducible mouse model of iRFP713 to track recombinase activity and tumour development in vivo.

First Author  Hock AK Year  2017
Journal  Sci Rep Volume  7
Issue  1 Pages  1837
PubMed ID  28500323 Mgi Jnum  J:282268
Mgi Id  MGI:6382341 Doi  10.1038/s41598-017-01741-0
Citation  Hock AK, et al. (2017) Development of an inducible mouse model of iRFP713 to track recombinase activity and tumour development in vivo. Sci Rep 7(1):1837
abstractText  While the use of bioluminescent proteins for molecular imaging is a powerful technology to further our understanding of complex processes, fluorescent labeling with visible light fluorescent proteins such as GFP and RFP suffers from poor tissue penetration and high background autofluorescence. To overcome these limitations, we generated an inducible knock-in mouse model of iRFP713. This model was used to assess Cre activity in a Rosa Cre-ER background and quantify Cre activity upon different tamoxifen treatments in several organs. We also show that iRFP can be readily detected in 3D organoid cultures, FACS analysis and in vivo tumour models. Taken together we demonstrate that iRFP713 is a progressive step in in vivo imaging and analysis that widens the optical imaging window to the near-infrared spectrum, thereby allowing deeper tissue penetration, quicker image acquisition without the need to inject substrates and a better signal to background ratio in genetically engineered mouse models (GEMMs).
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