JNK were not causally linked to the upregulation of Flt1 and Angpt2.We demonstrated that PKCinduced transcription of Angpt2 and Flt1 involved the transcription factor Ets1, as a combined knockdown of Fzd5 and Ets1 completely blocked the enhanced Angpt2 expression, and reduced the upregulation of Flt1 by almost 50% (both n¼4, P<0.05).In addition, an intervention with knockdown of Ets1 on top of the Fzd5 knockdown also partially rescued the poor angiogenic phenotype observed in the 3D co-culture model (n¼6, P<0.05), indicating that this transcription factor was critically involved in suppressing angiogenesis in absence of Fzd5.Conclusions: The current study provides evidence for a pro-angiogenic role of Fzd5, which was shown to be involved in endothelial tubule formation, cell cycle progression and migration, and does so by repression of PKC/Ets1-mediated transcription of Flt1 and Angpt2.
Deleted Author ID, Pallavi Chaturvedi, Sarah Krantz, Jennifer E. Klomp, Nicole M. Pohl-Avila, Anne‐Marie Ray, Péter T. Tóth, Peter Carmeliet, Andrei V. Karginov, Asrar B. Malik, Jalees Rehman
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