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Fibroblast growth factor receptor influences primary cilium length through an interaction with intestinal cell kinase
- Kunova Bosakova, Michaela;
- Nita, Alexandru;
- Gregor, Tomas;
- Varecha, Miroslav;
- Gudernova, Iva;
- Fafilek, Bohumil;
- Barta, Tomas;
- Basheer, Neha;
- Abraham, Sara P;
- Balek, Lukas;
- Tomanova, Marketa;
- Fialova Kucerova, Jana;
- Bosak, Juraj;
- Potesil, David;
- Zieba, Jennifer;
- Song, Jieun;
- Konik, Peter;
- Park, Sohyun;
- Duran, Ivan;
- Zdrahal, Zbynek;
- Smajs, David;
- Jansen, Gert;
- Fu, Zheng;
- Ko, Hyuk Wan;
- Hampl, Ales;
- Trantirek, Lukas;
- Krakow, Deborah;
- Krejci, Pavel
- et al.
Published Web Location
https://doi.org/10.1073/pnas.1800338116Abstract
Vertebrate primary cilium is a Hedgehog signaling center but the extent of its involvement in other signaling systems is less well understood. This report delineates a mechanism by which fibroblast growth factor (FGF) controls primary cilia. Employing proteomic approaches to characterize proteins associated with the FGF-receptor, FGFR3, we identified the serine/threonine kinase intestinal cell kinase (ICK) as an FGFR interactor. ICK is involved in ciliogenesis and participates in control of ciliary length. FGF signaling partially abolished ICK's kinase activity, through FGFR-mediated ICK phosphorylation at conserved residue Tyr15, which interfered with optimal ATP binding. Activation of the FGF signaling pathway affected both primary cilia length and function in a manner consistent with cilia effects caused by inhibition of ICK activity. Moreover, knockdown and knockout of ICK rescued the FGF-mediated effect on cilia. We provide conclusive evidence that FGF signaling controls cilia via interaction with ICK.
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