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Considerations for the use of Cre recombinase for conditional gene deletion in the mouse lens.

Phuong T LamStephanie L PadulaThanh V HoangJustin E PothLin LiuChun LiangAdam S LeFeverLindsay M WallaceRuth Ashery-PadanPenny K RiggsJordan E ShieldsOhad ShahamSheldon RowanNadean L BrownTom GlaserMichael L Robinson
Published in: Human genomics (2019)
Although P0-3.9GFPCre transgenic mice appear free from ocular abnormalities, extensive non-ocular CRE expression represents a potential problem for conditional gene deletion studies using this transgene. The higher level of CRE expression in Le-Cre lenses versus P0-3.9GFPCre lenses may explain abnormal lens development in homozygous Le-Cre mice. Given the lack of deregulation of PAX6-responsive transcripts, we suggest that abnormal eye development in Le-Cre transgenic mice stems from CRE toxicity. Our studies reinforce the requirement for appropriate CRE-only expressing controls when using CRE as a driver of conditional gene targeting strategies.
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