A genome-wide association study of sodium levels and drug metabolism in an epilepsy cohort treated with carbamazepine and oxcarbazepine

doi:10.1002/epi4.12297

A genome-wide association study of sodium levels and drug metabolism in an epilepsy cohort treated with carbamazepine and oxcarbazepine

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Abstract

Objective: To ascertain the clinical and genetic factors contributing to carbamazepine- and oxcarbazepine-induced hyponatremia (COIH), and to carbamazepine (CBZ) metabolism, in a retrospectively collected, cross-sectional cohort of people with epilepsy. Methods: We collected data on serum sodium levels and antiepileptic drug levels in people with epilepsy attending a tertiary epilepsy center while on treatment with CBZ or OXC. We defined hyponatremia as Na+ ≤134 mEq/L. We estimated the CBZ metabolic ratio defined as the log transformation of the ratio of metabolite CBZ-diol to unchanged drug precursor substrate as measured in serum. Results: Clinical and genetic data relating to carbamazepine and oxcarbazepine trials were collected in 1141 patients. We did not observe any genome-wide significant associations with sodium level in a linear trend or hyponatremia as a dichotomous trait. Age, sex, number of comedications, phenytoin use, phenobarbital use, and sodium valproate use were significant predictors of CBZ metabolic ratio. No genome-wide significant associations with CBZ metabolic ratio were found. Significance: Although we did not detect a genetic predictor of hyponatremia or CBZ metabolism in our cohort, our findings suggest that the determinants of CBZ metabolism are multifactorial.

Original language	English
Pages (from-to)	102-109
Number of pages	8
Journal	Epilepsia Open
Volume	4
Issue number	1
DOIs	https://doi.org/10.1002/epi4.12297
Publication status	Published - 1 Mar 2019

Keywords

adverse effects
antiepileptic drugs
EpiPGX Consortium
GWAS
hyponatremia

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@article{b80b712a6842472ba8e85dff0dfe9565,

title = "A genome-wide association study of sodium levels and drug metabolism in an epilepsy cohort treated with carbamazepine and oxcarbazepine",

abstract = "Objective: To ascertain the clinical and genetic factors contributing to carbamazepine- and oxcarbazepine-induced hyponatremia (COIH), and to carbamazepine (CBZ) metabolism, in a retrospectively collected, cross-sectional cohort of people with epilepsy. Methods: We collected data on serum sodium levels and antiepileptic drug levels in people with epilepsy attending a tertiary epilepsy center while on treatment with CBZ or OXC. We defined hyponatremia as Na+ ≤134 mEq/L. We estimated the CBZ metabolic ratio defined as the log transformation of the ratio of metabolite CBZ-diol to unchanged drug precursor substrate as measured in serum. Results: Clinical and genetic data relating to carbamazepine and oxcarbazepine trials were collected in 1141 patients. We did not observe any genome-wide significant associations with sodium level in a linear trend or hyponatremia as a dichotomous trait. Age, sex, number of comedications, phenytoin use, phenobarbital use, and sodium valproate use were significant predictors of CBZ metabolic ratio. No genome-wide significant associations with CBZ metabolic ratio were found. Significance: Although we did not detect a genetic predictor of hyponatremia or CBZ metabolism in our cohort, our findings suggest that the determinants of CBZ metabolism are multifactorial.",

keywords = "adverse effects, antiepileptic drugs, EpiPGX Consortium, GWAS, hyponatremia",

author = "Bianca Berghuis and Caragh Stapleton and Sonsma, {Anja C.M.} and Janic Hulst and {de Haan}, {Gerrit Jan} and Dick Lindhout and Rita Demurtas and Roland Krause and Chantal Depondt and Kunz, {Wolfram S.} and Federico Zara and Pasquale Striano and John Craig and Pauls Auce and Marson, {Anthony G.} and Hreinn Stefansson and O'Brien, {Terence J.} and Johnson, {Michael R.} and Sills, {Graeme J.} and Stefan Wolking and Holger Lerche and Sisodiya, {Sanjay M.} and Sander, {Josemir W.} and Cavalleri, {Gianpiero L.} and Koeleman, {Bobby P.C.} and Mark McCormack and A. Avbersek and C. Leu and K. Heggeli and J. Willis and D. Speed and N. Sargsyan and K. Chinthapalli and M. Borghei and A. Coppola and A. Gambardella and F. Becker and S. Rau and C. Hengsbach and Weber, {Y. G.} and N. Delanty and E. Campbell and Gudmundsson, {L. J.} and A. Ingason and K. Stef{\'a}nsson and R. Schneider and R. Balling and B. Francis and A. Jorgensen and A. Morris",

note = "Funding Information: Parts of the computational analysis were performed on the high-performance computer system of the University of Luxembourg (https://hpc.uni.lu). BB was supported by Christelijke Vereniging voor de Verpleging van Lijders aan Epilepsie, The Netherlands. MMC and GLC are supported by Science Foundation Ireland, grant 13/CDA/2223. MMC is supported by a Marie-Curie Individual Fellowship (No. 751761) from the European Commission. The EpiPGX Consortium was funded by FP7 Grant 279062 “EpiPGX” from the European Commission. SMS and JWS are based at the NIHR University College London Hospitals Comprehensive Biomedical Research Centre, which receives a proportion of funding from the UK Department of Health's Biomedical Research Centres{\textquoteright} funding scheme. SMS and JWS receive support the UK Epilepsy Society. JWS receives support from the Dr. Marvin Weil Epilepsy Research Fund. CPS receives support from the Irish Research Council and Punchestown Kidney Research fund (grant number EPSPG2015). Funding Information: Dr. Marvin Weil Epilepsy Research Fund; Irish Research Council for Science, Engineering and Technology; UK Department of Health's Biomedical Research Centre; H2020 Marie Sk{\l}odowska-Curie Actions, Grant/Award Number: 751761; Punchestown Kidney Research Fund, Grant/Award Number: EPSPG2015; Science Foundation Ireland, Grant/Award Number: 13/CDA/2223; Christelijke Vereniging voor de Verpleging van Lijders aan Epilepsie; Epilepsy Society Publisher Copyright: {\textcopyright} 2019 The Authors. Epilepsia Open published by Wiley Periodicals Inc. on behalf of International League Against Epilepsy.",

year = "2019",

month = mar,

day = "1",

doi = "10.1002/epi4.12297",

language = "English",

volume = "4",

pages = "102--109",

number = "1",

}

TY - JOUR

T1 - A genome-wide association study of sodium levels and drug metabolism in an epilepsy cohort treated with carbamazepine and oxcarbazepine

AU - Berghuis, Bianca

AU - Stapleton, Caragh

AU - Sonsma, Anja C.M.

AU - Hulst, Janic

AU - de Haan, Gerrit Jan

AU - Lindhout, Dick

AU - Demurtas, Rita

AU - Krause, Roland

AU - Depondt, Chantal

AU - Kunz, Wolfram S.

AU - Zara, Federico

AU - Striano, Pasquale

AU - Craig, John

AU - Auce, Pauls

AU - Marson, Anthony G.

AU - Stefansson, Hreinn

AU - O'Brien, Terence J.

AU - Johnson, Michael R.

AU - Sills, Graeme J.

AU - Wolking, Stefan

AU - Lerche, Holger

AU - Sisodiya, Sanjay M.

AU - Sander, Josemir W.

AU - Cavalleri, Gianpiero L.

AU - Koeleman, Bobby P.C.

AU - McCormack, Mark

AU - Avbersek, A.

AU - Leu, C.

AU - Heggeli, K.

AU - Willis, J.

AU - Speed, D.

AU - Sargsyan, N.

AU - Chinthapalli, K.

AU - Borghei, M.

AU - Coppola, A.

AU - Gambardella, A.

AU - Becker, F.

AU - Rau, S.

AU - Hengsbach, C.

AU - Weber, Y. G.

AU - Delanty, N.

AU - Campbell, E.

AU - Gudmundsson, L. J.

AU - Ingason, A.

AU - Stefánsson, K.

AU - Schneider, R.

AU - Balling, R.

AU - Francis, B.

AU - Jorgensen, A.

AU - Morris, A.

N1 - Funding Information: Parts of the computational analysis were performed on the high-performance computer system of the University of Luxembourg (https://hpc.uni.lu). BB was supported by Christelijke Vereniging voor de Verpleging van Lijders aan Epilepsie, The Netherlands. MMC and GLC are supported by Science Foundation Ireland, grant 13/CDA/2223. MMC is supported by a Marie-Curie Individual Fellowship (No. 751761) from the European Commission. The EpiPGX Consortium was funded by FP7 Grant 279062 “EpiPGX” from the European Commission. SMS and JWS are based at the NIHR University College London Hospitals Comprehensive Biomedical Research Centre, which receives a proportion of funding from the UK Department of Health's Biomedical Research Centres’ funding scheme. SMS and JWS receive support the UK Epilepsy Society. JWS receives support from the Dr. Marvin Weil Epilepsy Research Fund. CPS receives support from the Irish Research Council and Punchestown Kidney Research fund (grant number EPSPG2015). Funding Information: Dr. Marvin Weil Epilepsy Research Fund; Irish Research Council for Science, Engineering and Technology; UK Department of Health's Biomedical Research Centre; H2020 Marie Skłodowska-Curie Actions, Grant/Award Number: 751761; Punchestown Kidney Research Fund, Grant/Award Number: EPSPG2015; Science Foundation Ireland, Grant/Award Number: 13/CDA/2223; Christelijke Vereniging voor de Verpleging van Lijders aan Epilepsie; Epilepsy Society Publisher Copyright: © 2019 The Authors. Epilepsia Open published by Wiley Periodicals Inc. on behalf of International League Against Epilepsy.

PY - 2019/3/1

Y1 - 2019/3/1

N2 - Objective: To ascertain the clinical and genetic factors contributing to carbamazepine- and oxcarbazepine-induced hyponatremia (COIH), and to carbamazepine (CBZ) metabolism, in a retrospectively collected, cross-sectional cohort of people with epilepsy. Methods: We collected data on serum sodium levels and antiepileptic drug levels in people with epilepsy attending a tertiary epilepsy center while on treatment with CBZ or OXC. We defined hyponatremia as Na+ ≤134 mEq/L. We estimated the CBZ metabolic ratio defined as the log transformation of the ratio of metabolite CBZ-diol to unchanged drug precursor substrate as measured in serum. Results: Clinical and genetic data relating to carbamazepine and oxcarbazepine trials were collected in 1141 patients. We did not observe any genome-wide significant associations with sodium level in a linear trend or hyponatremia as a dichotomous trait. Age, sex, number of comedications, phenytoin use, phenobarbital use, and sodium valproate use were significant predictors of CBZ metabolic ratio. No genome-wide significant associations with CBZ metabolic ratio were found. Significance: Although we did not detect a genetic predictor of hyponatremia or CBZ metabolism in our cohort, our findings suggest that the determinants of CBZ metabolism are multifactorial.

AB - Objective: To ascertain the clinical and genetic factors contributing to carbamazepine- and oxcarbazepine-induced hyponatremia (COIH), and to carbamazepine (CBZ) metabolism, in a retrospectively collected, cross-sectional cohort of people with epilepsy. Methods: We collected data on serum sodium levels and antiepileptic drug levels in people with epilepsy attending a tertiary epilepsy center while on treatment with CBZ or OXC. We defined hyponatremia as Na+ ≤134 mEq/L. We estimated the CBZ metabolic ratio defined as the log transformation of the ratio of metabolite CBZ-diol to unchanged drug precursor substrate as measured in serum. Results: Clinical and genetic data relating to carbamazepine and oxcarbazepine trials were collected in 1141 patients. We did not observe any genome-wide significant associations with sodium level in a linear trend or hyponatremia as a dichotomous trait. Age, sex, number of comedications, phenytoin use, phenobarbital use, and sodium valproate use were significant predictors of CBZ metabolic ratio. No genome-wide significant associations with CBZ metabolic ratio were found. Significance: Although we did not detect a genetic predictor of hyponatremia or CBZ metabolism in our cohort, our findings suggest that the determinants of CBZ metabolism are multifactorial.

KW - adverse effects

KW - antiepileptic drugs

KW - EpiPGX Consortium

KW - GWAS

KW - hyponatremia

UR - http://www.scopus.com/inward/record.url?scp=85062408600&partnerID=8YFLogxK

U2 - 10.1002/epi4.12297

DO - 10.1002/epi4.12297

M3 - Article

AN - SCOPUS:85062408600

SN - 2470-9239

VL - 4

SP - 102

EP - 109

JO - Epilepsia Open

JF - Epilepsia Open

IS - 1

ER -

A genome-wide association study of sodium levels and drug metabolism in an epilepsy cohort treated with carbamazepine and oxcarbazepine

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Keywords

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