Mutations in KCNT1 cause a spectrum of focal epilepsies

Rikke S. Moller; Sarah E. Heron; Line H. G. Larsen; Chiao Xin Lim; Michael G. Ricos; Marta A. Bayly; Marjan J. A. van Kempen; Sylvia Klinkenberg; Ian Andrews; Kent Kelley; Gabriel M. Ronen; David Callen; Jacinta M. McMahon; Simone C. Yendle; Gemma L. Carvill; Heather C. Mefford; Rima Nabbout; Annapurna Poduri; Pasquale Striano; Maria G. Baglietto; Federico Zara; Nicholas J. Smith; Clair Pridmore; Elena Gardella; Marina Nikanorova; Hans Atli Dahl; Pia Gellert; Ingrid E. Scheffer; Boudewijn Gunning; Bente Kragh-Olsen; Leanne M. Dibbens

doi:10.1111/epi.13071

Mutations in KCNT1 cause a spectrum of focal epilepsies

Rikke S. Moller, Sarah E. Heron, Line H. G. Larsen, Chiao Xin Lim, Michael G. Ricos, Marta A. Bayly, Marjan J. A. van Kempen, Sylvia Klinkenberg, Ian Andrews, Kent Kelley, Gabriel M. Ronen, David Callen, Jacinta M. McMahon, Simone C. Yendle, Gemma L. Carvill, Heather C. Mefford, Rima Nabbout, Annapurna Poduri, Pasquale Striano, Maria G. BagliettoFederico Zara, Nicholas J. Smith, Clair Pridmore, Elena Gardella, Marina Nikanorova, Hans Atli Dahl, Pia Gellert, Ingrid E. Scheffer, Boudewijn Gunning, Bente Kragh-Olsen, Leanne M. Dibbens^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Autosomal dominant mutations in the sodium-gated potassium channel subunit gene KCNT1 have been associated with two distinct seizure syndromes, nocturnal frontal lobe epilepsy (NFLE) and malignant migrating focal seizures of infancy (MMFSI). To further explore the phenotypic spectrum associated with KCNT1, we examined individuals affected with focal epilepsy or an epileptic encephalopathy for mutations in the gene. We identified KCNT1 mutations in 12 previously unreported patients with focal epilepsy, multifocal epilepsy, cardiac arrhythmia, and in a family with sudden unexpected death in epilepsy (SUDEP), in addition to patients with NFLE and MMFSI. In contrast to the 100% penetrance so far reported for KCNT1 mutations, we observed incomplete penetrance. It is notable that we report that the one KCNT1 mutation, p.Arg398Gln, can lead to either of the two distinct phenotypes, ADNFLE or MMFSI, even within the same family. This indicates that genotype-phenotype relationships for KCNT1 mutations are not straightforward. We demonstrate that KCNT1 mutations are highly pleiotropic and are associated with phenotypes other than ADNFLE and MMFSI. KCNT1 mutations are now associated with Ohtahara syndrome, MMFSI, and nocturnal focal epilepsy. They may also be associated with multifocal epilepsy and cardiac disturbances.

Original language	English
Pages (from-to)	E114-E120
Journal	Epilepsia
Volume	56
Issue number	9
DOIs	https://doi.org/10.1111/epi.13071
Publication status	Published - Sept 2015

Keywords

KCNT1
Autosomal dominant nocturnal frontal lobe epilepsy
Epileptic encephalopathy
Cardiac arrhythmia
Sudden unexpected death in epilepsy

Access to Document

10.1111/epi.13071

Cite this

Moller, R. S., Heron, S. E., Larsen, L. H. G., Lim, C. X., Ricos, M. G., Bayly, M. A., van Kempen, M. J. A., Klinkenberg, S., Andrews, I., Kelley, K., Ronen, G. M., Callen, D., McMahon, J. M., Yendle, S. C., Carvill, G. L., Mefford, H. C., Nabbout, R., Poduri, A., Striano, P., ... Dibbens, L. M. (2015). Mutations in KCNT1 cause a spectrum of focal epilepsies. Epilepsia, 56(9), E114-E120. https://doi.org/10.1111/epi.13071

@article{03d8cf1dc65f465d9dcd548b6ae4510d,

title = "Mutations in KCNT1 cause a spectrum of focal epilepsies",

abstract = "Autosomal dominant mutations in the sodium-gated potassium channel subunit gene KCNT1 have been associated with two distinct seizure syndromes, nocturnal frontal lobe epilepsy (NFLE) and malignant migrating focal seizures of infancy (MMFSI). To further explore the phenotypic spectrum associated with KCNT1, we examined individuals affected with focal epilepsy or an epileptic encephalopathy for mutations in the gene. We identified KCNT1 mutations in 12 previously unreported patients with focal epilepsy, multifocal epilepsy, cardiac arrhythmia, and in a family with sudden unexpected death in epilepsy (SUDEP), in addition to patients with NFLE and MMFSI. In contrast to the 100% penetrance so far reported for KCNT1 mutations, we observed incomplete penetrance. It is notable that we report that the one KCNT1 mutation, p.Arg398Gln, can lead to either of the two distinct phenotypes, ADNFLE or MMFSI, even within the same family. This indicates that genotype-phenotype relationships for KCNT1 mutations are not straightforward. We demonstrate that KCNT1 mutations are highly pleiotropic and are associated with phenotypes other than ADNFLE and MMFSI. KCNT1 mutations are now associated with Ohtahara syndrome, MMFSI, and nocturnal focal epilepsy. They may also be associated with multifocal epilepsy and cardiac disturbances.",

keywords = "KCNT1, Autosomal dominant nocturnal frontal lobe epilepsy, Epileptic encephalopathy, Cardiac arrhythmia, Sudden unexpected death in epilepsy",

author = "Moller, {Rikke S.} and Heron, {Sarah E.} and Larsen, {Line H. G.} and Lim, {Chiao Xin} and Ricos, {Michael G.} and Bayly, {Marta A.} and {van Kempen}, {Marjan J. A.} and Sylvia Klinkenberg and Ian Andrews and Kent Kelley and Ronen, {Gabriel M.} and David Callen and McMahon, {Jacinta M.} and Yendle, {Simone C.} and Carvill, {Gemma L.} and Mefford, {Heather C.} and Rima Nabbout and Annapurna Poduri and Pasquale Striano and Baglietto, {Maria G.} and Federico Zara and Smith, {Nicholas J.} and Clair Pridmore and Elena Gardella and Marina Nikanorova and Dahl, {Hans Atli} and Pia Gellert and Scheffer, {Ingrid E.} and Boudewijn Gunning and Bente Kragh-Olsen and Dibbens, {Leanne M.}",

year = "2015",

month = sep,

doi = "10.1111/epi.13071",

language = "English",

volume = "56",

pages = "E114--E120",

journal = "Epilepsia",

issn = "0013-9580",

publisher = "Wiley",

number = "9",

}

Moller, RS, Heron, SE, Larsen, LHG, Lim, CX, Ricos, MG, Bayly, MA, van Kempen, MJA, Klinkenberg, S, Andrews, I, Kelley, K, Ronen, GM, Callen, D, McMahon, JM, Yendle, SC, Carvill, GL, Mefford, HC, Nabbout, R, Poduri, A, Striano, P, Baglietto, MG, Zara, F, Smith, NJ, Pridmore, C, Gardella, E, Nikanorova, M, Dahl, HA, Gellert, P, Scheffer, IE, Gunning, B, Kragh-Olsen, B & Dibbens, LM 2015, 'Mutations in KCNT1 cause a spectrum of focal epilepsies', Epilepsia, vol. 56, no. 9, pp. E114-E120. https://doi.org/10.1111/epi.13071

TY - JOUR

T1 - Mutations in KCNT1 cause a spectrum of focal epilepsies

AU - Moller, Rikke S.

AU - Heron, Sarah E.

AU - Larsen, Line H. G.

AU - Lim, Chiao Xin

AU - Ricos, Michael G.

AU - Bayly, Marta A.

AU - van Kempen, Marjan J. A.

AU - Klinkenberg, Sylvia

AU - Andrews, Ian

AU - Kelley, Kent

AU - Ronen, Gabriel M.

AU - Callen, David

AU - McMahon, Jacinta M.

AU - Yendle, Simone C.

AU - Carvill, Gemma L.

AU - Mefford, Heather C.

AU - Nabbout, Rima

AU - Poduri, Annapurna

AU - Striano, Pasquale

AU - Baglietto, Maria G.

AU - Zara, Federico

AU - Smith, Nicholas J.

AU - Pridmore, Clair

AU - Gardella, Elena

AU - Nikanorova, Marina

AU - Dahl, Hans Atli

AU - Gellert, Pia

AU - Scheffer, Ingrid E.

AU - Gunning, Boudewijn

AU - Kragh-Olsen, Bente

AU - Dibbens, Leanne M.

PY - 2015/9

Y1 - 2015/9

N2 - Autosomal dominant mutations in the sodium-gated potassium channel subunit gene KCNT1 have been associated with two distinct seizure syndromes, nocturnal frontal lobe epilepsy (NFLE) and malignant migrating focal seizures of infancy (MMFSI). To further explore the phenotypic spectrum associated with KCNT1, we examined individuals affected with focal epilepsy or an epileptic encephalopathy for mutations in the gene. We identified KCNT1 mutations in 12 previously unreported patients with focal epilepsy, multifocal epilepsy, cardiac arrhythmia, and in a family with sudden unexpected death in epilepsy (SUDEP), in addition to patients with NFLE and MMFSI. In contrast to the 100% penetrance so far reported for KCNT1 mutations, we observed incomplete penetrance. It is notable that we report that the one KCNT1 mutation, p.Arg398Gln, can lead to either of the two distinct phenotypes, ADNFLE or MMFSI, even within the same family. This indicates that genotype-phenotype relationships for KCNT1 mutations are not straightforward. We demonstrate that KCNT1 mutations are highly pleiotropic and are associated with phenotypes other than ADNFLE and MMFSI. KCNT1 mutations are now associated with Ohtahara syndrome, MMFSI, and nocturnal focal epilepsy. They may also be associated with multifocal epilepsy and cardiac disturbances.

AB - Autosomal dominant mutations in the sodium-gated potassium channel subunit gene KCNT1 have been associated with two distinct seizure syndromes, nocturnal frontal lobe epilepsy (NFLE) and malignant migrating focal seizures of infancy (MMFSI). To further explore the phenotypic spectrum associated with KCNT1, we examined individuals affected with focal epilepsy or an epileptic encephalopathy for mutations in the gene. We identified KCNT1 mutations in 12 previously unreported patients with focal epilepsy, multifocal epilepsy, cardiac arrhythmia, and in a family with sudden unexpected death in epilepsy (SUDEP), in addition to patients with NFLE and MMFSI. In contrast to the 100% penetrance so far reported for KCNT1 mutations, we observed incomplete penetrance. It is notable that we report that the one KCNT1 mutation, p.Arg398Gln, can lead to either of the two distinct phenotypes, ADNFLE or MMFSI, even within the same family. This indicates that genotype-phenotype relationships for KCNT1 mutations are not straightforward. We demonstrate that KCNT1 mutations are highly pleiotropic and are associated with phenotypes other than ADNFLE and MMFSI. KCNT1 mutations are now associated with Ohtahara syndrome, MMFSI, and nocturnal focal epilepsy. They may also be associated with multifocal epilepsy and cardiac disturbances.

KW - KCNT1

KW - Autosomal dominant nocturnal frontal lobe epilepsy

KW - Epileptic encephalopathy

KW - Cardiac arrhythmia

KW - Sudden unexpected death in epilepsy

U2 - 10.1111/epi.13071

DO - 10.1111/epi.13071

M3 - Article

C2 - 26122718

SN - 0013-9580

VL - 56

SP - E114-E120

JO - Epilepsia

JF - Epilepsia

IS - 9

ER -