Mosaicism of de novo pathogenic SCN1A variants in epilepsy is a frequent phenomenon that correlates with variable phenotypes

Iris M. de Lange; Marco J. Koudijs; Ruben van 't Slot; Boudewijn Gunning; Anja C.M. Sonsma; Lisette J.J.M. van Gemert; Flip Mulder; Ellen C. Carbo; Marjan J.A. van Kempen; Nienke E. Verbeek; Isaac J. Nijman; Robert F. Ernst; Sanne M.C. Savelberg; Nine V.A.M. Knoers; Eva H. Brilstra; Bobby P.C. Koeleman

doi:10.1111/epi.14021

Mosaicism of de novo pathogenic SCN1A variants in epilepsy is a frequent phenomenon that correlates with variable phenotypes

Iris M. de Lange^*, Marco J. Koudijs, Ruben van 't Slot, Boudewijn Gunning, Anja C.M. Sonsma, Lisette J.J.M. van Gemert, Flip Mulder, Ellen C. Carbo, Marjan J.A. van Kempen, Nienke E. Verbeek, Isaac J. Nijman, Robert F. Ernst, Sanne M.C. Savelberg, Nine V.A.M. Knoers, Eva H. Brilstra, Bobby P.C. Koeleman

^*Corresponding author for this work

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

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Abstract

Objective: Phenotypes caused by de novo SCN1A pathogenic variants are very variable, ranging from severely affected patients with Dravet syndrome to much milder genetic epilepsy febrile seizures plus cases. The most important determinant of disease severity is the type of variant, with variants that cause a complete loss of function of the SCN1A protein (α-subunit of the neuronal sodium channel Nav1.1) being detected almost exclusively in Dravet syndrome patients. However, even within Dravet syndrome disease severity ranges greatly, and consequently other disease modifiers must exist. A better prediction of disease severity is very much needed in daily practice to improve counseling, stressing the importance of identifying modifying factors in this patient group. We evaluated 128 participants with de novo, pathogenic SCN1A variants to investigate whether mosaicism, caused by postzygotic mutation, is a major modifier in SCN1A-related epilepsy. Methods: Mosaicism was investigated by reanalysis of the pathogenic SCN1A variants using single molecule molecular inversion probes and next generation sequencing with high coverage. Allelic ratios of pathogenic variants were used to determine whether mosaicism was likely. Selected mosaic variants were confirmed by droplet digital polymerase chain reaction and sequencing of different tissues. Developmental outcome was classified based on available data on intelligence quotient and school functioning/education. Results: Mosaicism was present for 7.5% of de novo pathogenic SCN1A variants in symptomatic patients. Mosaic participants were less severely affected than nonmosaic participants if only participants with truncating variants are considered (distribution of developmental outcome scores, Mann-Whitney U, P =.023). Significance: Postzygotic mutation is a common phenomenon in SCN1A-related epilepsies. Participants with mosaicism have on average milder phenotypes, suggesting that mosaicism can be a major modifier of SCN1A-related diseases. Detection of mosaicism has important implications for genetic counseling and can be achieved by deep sequencing of unique reads.

Original language	English
Pages (from-to)	690-703
Number of pages	14
Journal	Epilepsia
Volume	59
Issue number	3
DOIs	https://doi.org/10.1111/epi.14021
Publication status	Published - 1 Mar 2018

Keywords

Dravet syndrome
epilepsy
mosaicism
postzygotic mutation
SCN1A

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de Lange, I. M., Koudijs, M. J., van 't Slot, R., Gunning, B., Sonsma, A. C. M., van Gemert, L. J. J. M., Mulder, F., Carbo, E. C., van Kempen, M. J. A., Verbeek, N. E., Nijman, I. J., Ernst, R. F., Savelberg, S. M. C., Knoers, N. V. A. M., Brilstra, E. H., & Koeleman, B. P. C. (2018). Mosaicism of de novo pathogenic SCN1A variants in epilepsy is a frequent phenomenon that correlates with variable phenotypes. Epilepsia, 59(3), 690-703. https://doi.org/10.1111/epi.14021

@article{b6a53e36d4334e6b853132e8c717b65f,

title = "Mosaicism of de novo pathogenic SCN1A variants in epilepsy is a frequent phenomenon that correlates with variable phenotypes",

abstract = "Objective: Phenotypes caused by de novo SCN1A pathogenic variants are very variable, ranging from severely affected patients with Dravet syndrome to much milder genetic epilepsy febrile seizures plus cases. The most important determinant of disease severity is the type of variant, with variants that cause a complete loss of function of the SCN1A protein (α-subunit of the neuronal sodium channel Nav1.1) being detected almost exclusively in Dravet syndrome patients. However, even within Dravet syndrome disease severity ranges greatly, and consequently other disease modifiers must exist. A better prediction of disease severity is very much needed in daily practice to improve counseling, stressing the importance of identifying modifying factors in this patient group. We evaluated 128 participants with de novo, pathogenic SCN1A variants to investigate whether mosaicism, caused by postzygotic mutation, is a major modifier in SCN1A-related epilepsy. Methods: Mosaicism was investigated by reanalysis of the pathogenic SCN1A variants using single molecule molecular inversion probes and next generation sequencing with high coverage. Allelic ratios of pathogenic variants were used to determine whether mosaicism was likely. Selected mosaic variants were confirmed by droplet digital polymerase chain reaction and sequencing of different tissues. Developmental outcome was classified based on available data on intelligence quotient and school functioning/education. Results: Mosaicism was present for 7.5% of de novo pathogenic SCN1A variants in symptomatic patients. Mosaic participants were less severely affected than nonmosaic participants if only participants with truncating variants are considered (distribution of developmental outcome scores, Mann-Whitney U, P =.023). Significance: Postzygotic mutation is a common phenomenon in SCN1A-related epilepsies. Participants with mosaicism have on average milder phenotypes, suggesting that mosaicism can be a major modifier of SCN1A-related diseases. Detection of mosaicism has important implications for genetic counseling and can be achieved by deep sequencing of unique reads.",

keywords = "Dravet syndrome, epilepsy, mosaicism, postzygotic mutation, SCN1A",

author = "{de Lange}, {Iris M.} and Koudijs, {Marco J.} and {van 't Slot}, Ruben and Boudewijn Gunning and Sonsma, {Anja C.M.} and {van Gemert}, {Lisette J.J.M.} and Flip Mulder and Carbo, {Ellen C.} and {van Kempen}, {Marjan J.A.} and Verbeek, {Nienke E.} and Nijman, {Isaac J.} and Ernst, {Robert F.} and Savelberg, {Sanne M.C.} and Knoers, {Nine V.A.M.} and Brilstra, {Eva H.} and Koeleman, {Bobby P.C.}",

note = "Publisher Copyright: {\textcopyright} 2018 The Authors. Epilepsia published by Wiley Periodicals, Inc. on behalf of International League Against Epilepsy",

year = "2018",

month = mar,

day = "1",

doi = "10.1111/epi.14021",

language = "English",

volume = "59",

pages = "690--703",

journal = "Epilepsia",

issn = "0013-9580",

publisher = "Wiley-Blackwell",

number = "3",

}

de Lange, IM, Koudijs, MJ, van 't Slot, R, Gunning, B, Sonsma, ACM, van Gemert, LJJM, Mulder, F, Carbo, EC, van Kempen, MJA, Verbeek, NE, Nijman, IJ, Ernst, RF, Savelberg, SMC, Knoers, NVAM, Brilstra, EH & Koeleman, BPC 2018, 'Mosaicism of de novo pathogenic SCN1A variants in epilepsy is a frequent phenomenon that correlates with variable phenotypes', Epilepsia, vol. 59, no. 3, pp. 690-703. https://doi.org/10.1111/epi.14021

TY - JOUR

T1 - Mosaicism of de novo pathogenic SCN1A variants in epilepsy is a frequent phenomenon that correlates with variable phenotypes

AU - de Lange, Iris M.

AU - Koudijs, Marco J.

AU - van 't Slot, Ruben

AU - Gunning, Boudewijn

AU - Sonsma, Anja C.M.

AU - van Gemert, Lisette J.J.M.

AU - Mulder, Flip

AU - Carbo, Ellen C.

AU - van Kempen, Marjan J.A.

AU - Verbeek, Nienke E.

AU - Nijman, Isaac J.

AU - Ernst, Robert F.

AU - Savelberg, Sanne M.C.

AU - Knoers, Nine V.A.M.

AU - Brilstra, Eva H.

AU - Koeleman, Bobby P.C.

PY - 2018/3/1

Y1 - 2018/3/1

N2 - Objective: Phenotypes caused by de novo SCN1A pathogenic variants are very variable, ranging from severely affected patients with Dravet syndrome to much milder genetic epilepsy febrile seizures plus cases. The most important determinant of disease severity is the type of variant, with variants that cause a complete loss of function of the SCN1A protein (α-subunit of the neuronal sodium channel Nav1.1) being detected almost exclusively in Dravet syndrome patients. However, even within Dravet syndrome disease severity ranges greatly, and consequently other disease modifiers must exist. A better prediction of disease severity is very much needed in daily practice to improve counseling, stressing the importance of identifying modifying factors in this patient group. We evaluated 128 participants with de novo, pathogenic SCN1A variants to investigate whether mosaicism, caused by postzygotic mutation, is a major modifier in SCN1A-related epilepsy. Methods: Mosaicism was investigated by reanalysis of the pathogenic SCN1A variants using single molecule molecular inversion probes and next generation sequencing with high coverage. Allelic ratios of pathogenic variants were used to determine whether mosaicism was likely. Selected mosaic variants were confirmed by droplet digital polymerase chain reaction and sequencing of different tissues. Developmental outcome was classified based on available data on intelligence quotient and school functioning/education. Results: Mosaicism was present for 7.5% of de novo pathogenic SCN1A variants in symptomatic patients. Mosaic participants were less severely affected than nonmosaic participants if only participants with truncating variants are considered (distribution of developmental outcome scores, Mann-Whitney U, P =.023). Significance: Postzygotic mutation is a common phenomenon in SCN1A-related epilepsies. Participants with mosaicism have on average milder phenotypes, suggesting that mosaicism can be a major modifier of SCN1A-related diseases. Detection of mosaicism has important implications for genetic counseling and can be achieved by deep sequencing of unique reads.

AB - Objective: Phenotypes caused by de novo SCN1A pathogenic variants are very variable, ranging from severely affected patients with Dravet syndrome to much milder genetic epilepsy febrile seizures plus cases. The most important determinant of disease severity is the type of variant, with variants that cause a complete loss of function of the SCN1A protein (α-subunit of the neuronal sodium channel Nav1.1) being detected almost exclusively in Dravet syndrome patients. However, even within Dravet syndrome disease severity ranges greatly, and consequently other disease modifiers must exist. A better prediction of disease severity is very much needed in daily practice to improve counseling, stressing the importance of identifying modifying factors in this patient group. We evaluated 128 participants with de novo, pathogenic SCN1A variants to investigate whether mosaicism, caused by postzygotic mutation, is a major modifier in SCN1A-related epilepsy. Methods: Mosaicism was investigated by reanalysis of the pathogenic SCN1A variants using single molecule molecular inversion probes and next generation sequencing with high coverage. Allelic ratios of pathogenic variants were used to determine whether mosaicism was likely. Selected mosaic variants were confirmed by droplet digital polymerase chain reaction and sequencing of different tissues. Developmental outcome was classified based on available data on intelligence quotient and school functioning/education. Results: Mosaicism was present for 7.5% of de novo pathogenic SCN1A variants in symptomatic patients. Mosaic participants were less severely affected than nonmosaic participants if only participants with truncating variants are considered (distribution of developmental outcome scores, Mann-Whitney U, P =.023). Significance: Postzygotic mutation is a common phenomenon in SCN1A-related epilepsies. Participants with mosaicism have on average milder phenotypes, suggesting that mosaicism can be a major modifier of SCN1A-related diseases. Detection of mosaicism has important implications for genetic counseling and can be achieved by deep sequencing of unique reads.

KW - Dravet syndrome

KW - epilepsy

KW - mosaicism

KW - postzygotic mutation

KW - SCN1A

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U2 - 10.1111/epi.14021

DO - 10.1111/epi.14021

M3 - Article

C2 - 29460957

SN - 0013-9580

VL - 59

SP - 690

EP - 703

JO - Epilepsia

JF - Epilepsia

IS - 3

ER -

Mosaicism of de novo pathogenic SCN1A variants in epilepsy is a frequent phenomenon that correlates with variable phenotypes

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Keywords

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