CK2 activity is required for the interaction of FGF14 with voltage-gated sodium channels and neuronal excitability

Hsu, Wei-Chun J; Scala, Federico; Nenov, Miroslav N; Wildburger, Norelle C; Elferink, Hannah; Singh, Aditya K; Chesson, Charles B; Buzhdygan, Tetyana; Sohail, Maveen; Shavkunov, Alexander S; Panova, Neli I; Nilsson, Carol L.; Rudra, Jai S; Lichti, Cheryl F; Laezza, Fernanda

CK2 activity is required for the interaction of FGF14 with voltage-gated sodium channels and neuronal excitability

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Hsu, Wei-Chun J ; Scala, Federico ; Nenov, Miroslav N ; Wildburger, Norelle C ; Elferink, Hannah ; Singh, Aditya K ; Chesson, Charles B ; Buzhdygan, Tetyana ; Sohail, Maveen and Shavkunov, Alexander S , et al. (2016) In FASEB Journal 30(6). p.86-2171

Abstract: Recent data shows that fibroblast growth factor 14 (FGF14) binds to and controls the function of the voltage-gated sodium (Nav) channel with phenotypic outcomes on neuronal excitability. Mutations in the FGF14 gene in humans have been associated with brain disorders that are partially recapitulated in Fgf14(-/-) mice. Thus, signaling pathways that modulate the FGF14:Nav channel interaction may be important therapeutic targets. Bioluminescence-based screening of small molecule modulators of the FGF14:Nav1.6 complex identified 4,5,6,7 -: tetrabromobenzotriazole (TBB), a potent casein kinase 2 (CK2) inhibitor, as a strong suppressor of FGF14:Nav1.6 interaction. Inhibition of CK2 through TBB reduces the interaction of FGF14 with Nav1.6 and... (More); Recent data shows that fibroblast growth factor 14 (FGF14) binds to and controls the function of the voltage-gated sodium (Nav) channel with phenotypic outcomes on neuronal excitability. Mutations in the FGF14 gene in humans have been associated with brain disorders that are partially recapitulated in Fgf14(-/-) mice. Thus, signaling pathways that modulate the FGF14:Nav channel interaction may be important therapeutic targets. Bioluminescence-based screening of small molecule modulators of the FGF14:Nav1.6 complex identified 4,5,6,7 -: tetrabromobenzotriazole (TBB), a potent casein kinase 2 (CK2) inhibitor, as a strong suppressor of FGF14:Nav1.6 interaction. Inhibition of CK2 through TBB reduces the interaction of FGF14 with Nav1.6 and Nav1.2 channels. Mass spectrometry confirmed direct phosphorylation of FGF14 by CK2 at S228 and S230, and mutation to alanine at these sites modified FGF14 modulation of Nav1.6-mediated currents. In 1 d in vitro hippocampal neurons, TBB induced a reduction in FGF14 expression, a decrease in transient Na(+) current amplitude, and a hyperpolarizing shift in the voltage dependence of Nav channel steady-state inactivation. In mature neurons, TBB reduces the axodendritic polarity of FGF14. In cornu ammonis area 1 hippocampal slices from wild-type mice, TBB impairs neuronal excitability by increasing action potential threshold and lowering firing frequency. Importantly, these changes in excitability are recapitulated in Fgf14(-/-) mice, and deletion of Fgf14 occludes TBB-dependent phenotypes observed in wild-type mice. These results suggest that a CK2-FGF14 axis may regulate Nav channels and neuronal excitability.-Hsu, W.-C. J., Scala, F., Nenov, M. N., Wildburger, N. C., Elferink, H., Singh, A. K., Chesson, C. B., Buzhdygan, T., Sohail, M., Shavkunov, A. S., Panova, N. I., Nilsson, C. L., Rudra, J. S., Lichti, C. F., Laezza, F. CK2 activity is required for the interaction of FGF14 with voltage-gated sodium channels and neuronal excitability.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/0cd2d581-64b3-452d-b877-d38c9e1758fe

author

Hsu, Wei-Chun J ; Scala, Federico ; Nenov, Miroslav N ; Wildburger, Norelle C ; Elferink, Hannah ; Singh, Aditya K ; Chesson, Charles B ; Buzhdygan, Tetyana ; Sohail, Maveen and Shavkunov, Alexander S , et al. (More)

Hsu, Wei-Chun J ; Scala, Federico ; Nenov, Miroslav N ; Wildburger, Norelle C ; Elferink, Hannah ; Singh, Aditya K ; Chesson, Charles B ; Buzhdygan, Tetyana ; Sohail, Maveen ; Shavkunov, Alexander S ; Panova, Neli I ; Nilsson, Carol L. ^LU ; Rudra, Jai S ; Lichti, Cheryl F and Laezza, Fernanda (Less)

publishing date

2016-06

type

Contribution to journal

publication status

published

in

FASEB Journal

volume

30

issue

6

pages

16 pages

publisher

Wiley

external identifiers

pmid:26917740
scopus:84971670334

ISSN

1530-6860

DOI

10.1096/fj.201500161

language

English

LU publication?

no

id

0cd2d581-64b3-452d-b877-d38c9e1758fe

date added to LUP

2017-05-16 10:18:49

date last changed

2024-06-09 16:34:09

@article{0cd2d581-64b3-452d-b877-d38c9e1758fe,
  abstract     = {{<p>Recent data shows that fibroblast growth factor 14 (FGF14) binds to and controls the function of the voltage-gated sodium (Nav) channel with phenotypic outcomes on neuronal excitability. Mutations in the FGF14 gene in humans have been associated with brain disorders that are partially recapitulated in Fgf14(-/-) mice. Thus, signaling pathways that modulate the FGF14:Nav channel interaction may be important therapeutic targets. Bioluminescence-based screening of small molecule modulators of the FGF14:Nav1.6 complex identified 4,5,6,7 -: tetrabromobenzotriazole (TBB), a potent casein kinase 2 (CK2) inhibitor, as a strong suppressor of FGF14:Nav1.6 interaction. Inhibition of CK2 through TBB reduces the interaction of FGF14 with Nav1.6 and Nav1.2 channels. Mass spectrometry confirmed direct phosphorylation of FGF14 by CK2 at S228 and S230, and mutation to alanine at these sites modified FGF14 modulation of Nav1.6-mediated currents. In 1 d in vitro hippocampal neurons, TBB induced a reduction in FGF14 expression, a decrease in transient Na(+) current amplitude, and a hyperpolarizing shift in the voltage dependence of Nav channel steady-state inactivation. In mature neurons, TBB reduces the axodendritic polarity of FGF14. In cornu ammonis area 1 hippocampal slices from wild-type mice, TBB impairs neuronal excitability by increasing action potential threshold and lowering firing frequency. Importantly, these changes in excitability are recapitulated in Fgf14(-/-) mice, and deletion of Fgf14 occludes TBB-dependent phenotypes observed in wild-type mice. These results suggest that a CK2-FGF14 axis may regulate Nav channels and neuronal excitability.-Hsu, W.-C. J., Scala, F., Nenov, M. N., Wildburger, N. C., Elferink, H., Singh, A. K., Chesson, C. B., Buzhdygan, T., Sohail, M., Shavkunov, A. S., Panova, N. I., Nilsson, C. L., Rudra, J. S., Lichti, C. F., Laezza, F. CK2 activity is required for the interaction of FGF14 with voltage-gated sodium channels and neuronal excitability.</p>}},
  author       = {{Hsu, Wei-Chun J and Scala, Federico and Nenov, Miroslav N and Wildburger, Norelle C and Elferink, Hannah and Singh, Aditya K and Chesson, Charles B and Buzhdygan, Tetyana and Sohail, Maveen and Shavkunov, Alexander S and Panova, Neli I and Nilsson, Carol L. and Rudra, Jai S and Lichti, Cheryl F and Laezza, Fernanda}},
  issn         = {{1530-6860}},
  language     = {{eng}},
  number       = {{6}},
  pages        = {{86--2171}},
  publisher    = {{Wiley}},
  series       = {{FASEB Journal}},
  title        = {{CK2 activity is required for the interaction of FGF14 with voltage-gated sodium channels and neuronal excitability}},
  url          = {{http://dx.doi.org/10.1096/fj.201500161}},
  doi          = {{10.1096/fj.201500161}},
  volume       = {{30}},
  year         = {{2016}},
}

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CK2 activity is required for the interaction of FGF14 with voltage-gated sodium channels and neuronal excitability