Lamotrigine use in pregnancy and risk of orofacial cleft, an update of eurocat lamotrigine study

Hao Wang; Maria Loane; Ester Garne; Joan Morris; Vera Nelen; Babak Khoshnood; Anke Rißmann; Awi Wiesel; Mary O'Mahony; Anna Pierini; Elisa Calzolari; Miriam Gatt; Marian Bakker; Marie-Claude Addor; David Tucker; Kari Klungsoyr; Anna Latos-Bielenska; Jan P. Mejnartowicz; Karin Kallen; Ingeborg Barisic; Christine Verellen-Dumoulin; Bérénice Doray; Larraitz Arriola; Diana Wellesley; Amanda Neville; Lolkje T.W. De Jong-Van Den Berg; Helen Dolk

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Background: Lamotrigine (LTG) is increasingly used during pregnancy. A FDA warning was issued for an association of LTG exposure and increased risk of orofacial clefts (OCs), based on data from the North American Antiepileptic Drug Pregnancy Registry (Holmes, 2006; Holmes et al., 2008). The signal was examined in the European Surveillance of Congenital Anomalies (EUROCAT) antiepileptic-study database (Dolk, 2008). No significantly increased risk of OCs was found relative to other malformations, either for isolated orofacial clefts or for isolated cleft palate. There has been no independent confirmation of increased risk of OCs in relation to LTG from all studies in the literature combined (Dolk et al., 2012). Objectives: To investigate whether first trimester exposure to LTG monotherapy is specifically associated with an increased risk of OCs, using the EUROCAT antiepilepticstudy database including birth years up to 2010. Methods: A population-based case-control study with malformed controls was performed. The updated EUROCAT antiepileptic-study dataset included 226,806 live births, stillbirths, or terminations with malformations among 7.6 million births in 20 European countries from 1995 to 2010, more than twice the population of the original study. Cases were 10,523 nonsyndromic OC registrations, of whom 8,771 were isolated, and 3,789 cleft palate (CP) of whom 2,984 were isolated. Controls were 144,914 non-chromosomal, non-OC registrations. We compared first trimester LTG vs no antiepileptics (non- AED use), for mono and polytherapy. Results: There were 181 LTG exposed (109 mono- and 72 polytherapy) registrations. Thematernal age adjusted odds ratios (ORs) for LTG monotherapy vs non-AED use were 0.84 (95% CI 0.37-1.92) for OC relative to other malformations, 1.01 (95% CI 0.44-2.30) for isolated OC; 1.18 (95% CI 0.38-3.72) for CP, and 1.49 (95% CI 0.47-4.72) for isolated CP. Conclusions: This update does not change the conclusion of the original study: we found no evidence of an increased risk of isolated orofacial clefts relative to other malformations for LTG monotherapy exposure in the first trimester, nor any evidence of an increased risk for isolated cleft palate.

Originele taal-2	English
Pagina's (van-tot)	304
Aantal pagina's	1
Tijdschrift	Pharmacoepidemiology and Drug Safety
Volume	23
Status	Published - 1-okt.-2014

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https://onlinelibrary.wiley.com/doi/10.1002/pds.3701

EUROCAT Northern Netherlands
Broekstra, D. (Supervisor), Kammen-Bergman, van, J. (Contributor), Bakker, M. (Contributor), Lutke, L. (Contributor), Doornbos, F. (Contributor), Smeijer-Ramocha, L. (Data Manager), van der Woude, A. (Contributor), de Walle, H. (Contributor) & Muhlenberg, N. (Data Manager), University of Groningen, 1981
DOI: 10.34760/5f5b80ff2a7a4, http://eurocat.umcg.nl
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Wang, H., Loane, M., Garne, E., Morris, J., Nelen, V., Khoshnood, B., Rißmann, A., Wiesel, A., O'Mahony, M., Pierini, A., Calzolari, E., Gatt, M., Bakker, M., Addor, M.-C., Tucker, D., Klungsoyr, K., Latos-Bielenska, A., Mejnartowicz, J. P., Kallen, K., ... Dolk, H. (2014). Lamotrigine use in pregnancy and risk of orofacial cleft, an update of eurocat lamotrigine study. Pharmacoepidemiology and Drug Safety, 23, 304.

@article{e1da774b02c64c5e87318860d39a03de,

title = "Lamotrigine use in pregnancy and risk of orofacial cleft, an update of eurocat lamotrigine study",

abstract = "Background: Lamotrigine (LTG) is increasingly used during pregnancy. A FDA warning was issued for an association of LTG exposure and increased risk of orofacial clefts (OCs), based on data from the North American Antiepileptic Drug Pregnancy Registry (Holmes, 2006; Holmes et al., 2008). The signal was examined in the European Surveillance of Congenital Anomalies (EUROCAT) antiepileptic-study database (Dolk, 2008). No significantly increased risk of OCs was found relative to other malformations, either for isolated orofacial clefts or for isolated cleft palate. There has been no independent confirmation of increased risk of OCs in relation to LTG from all studies in the literature combined (Dolk et al., 2012). Objectives: To investigate whether first trimester exposure to LTG monotherapy is specifically associated with an increased risk of OCs, using the EUROCAT antiepilepticstudy database including birth years up to 2010. Methods: A population-based case-control study with malformed controls was performed. The updated EUROCAT antiepileptic-study dataset included 226,806 live births, stillbirths, or terminations with malformations among 7.6 million births in 20 European countries from 1995 to 2010, more than twice the population of the original study. Cases were 10,523 nonsyndromic OC registrations, of whom 8,771 were isolated, and 3,789 cleft palate (CP) of whom 2,984 were isolated. Controls were 144,914 non-chromosomal, non-OC registrations. We compared first trimester LTG vs no antiepileptics (non- AED use), for mono and polytherapy. Results: There were 181 LTG exposed (109 mono- and 72 polytherapy) registrations. Thematernal age adjusted odds ratios (ORs) for LTG monotherapy vs non-AED use were 0.84 (95% CI 0.37-1.92) for OC relative to other malformations, 1.01 (95% CI 0.44-2.30) for isolated OC; 1.18 (95% CI 0.38-3.72) for CP, and 1.49 (95% CI 0.47-4.72) for isolated CP. Conclusions: This update does not change the conclusion of the original study: we found no evidence of an increased risk of isolated orofacial clefts relative to other malformations for LTG monotherapy exposure in the first trimester, nor any evidence of an increased risk for isolated cleft palate.",

keywords = "lamotrigine, anticonvulsive agent, pharmacoepidemiology, risk management, risk, pregnancy, congenital malformation, registration, monotherapy, cleft palate, first trimester pregnancy, exposure, data base, therapy, population, stillbirth, live birth, population based case control study, human, register, food and drug administration",

author = "Hao Wang and Maria Loane and Ester Garne and Joan Morris and Vera Nelen and Babak Khoshnood and Anke Ri{\ss}mann and Awi Wiesel and Mary O'Mahony and Anna Pierini and Elisa Calzolari and Miriam Gatt and Marian Bakker and Marie-Claude Addor and David Tucker and Kari Klungsoyr and Anna Latos-Bielenska and Mejnartowicz, {Jan P.} and Karin Kallen and Ingeborg Barisic and Christine Verellen-Dumoulin and B{\'e}r{\'e}nice Doray and Larraitz Arriola and Diana Wellesley and Amanda Neville and {De Jong-Van Den Berg}, {Lolkje T.W.} and Helen Dolk",

year = "2014",

month = oct,

day = "1",

language = "English",

volume = "23",

pages = "304",

journal = "Pharmacoepidemiology and Drug Safety",

issn = "1053-8569",

publisher = "Wiley",

}

Wang, H, Loane, M, Garne, E, Morris, J, Nelen, V, Khoshnood, B, Rißmann, A, Wiesel, A, O'Mahony, M, Pierini, A, Calzolari, E, Gatt, M, Bakker, M, Addor, M-C, Tucker, D, Klungsoyr, K, Latos-Bielenska, A, Mejnartowicz, JP, Kallen, K, Barisic, I, Verellen-Dumoulin, C, Doray, B, Arriola, L, Wellesley, D, Neville, A, De Jong-Van Den Berg, LTW & Dolk, H 2014, 'Lamotrigine use in pregnancy and risk of orofacial cleft, an update of eurocat lamotrigine study', Pharmacoepidemiology and Drug Safety, vol. 23, blz. 304.

TY - JOUR

T1 - Lamotrigine use in pregnancy and risk of orofacial cleft, an update of eurocat lamotrigine study

AU - Wang, Hao

AU - Loane, Maria

AU - Garne, Ester

AU - Morris, Joan

AU - Nelen, Vera

AU - Khoshnood, Babak

AU - Rißmann, Anke

AU - Wiesel, Awi

AU - O'Mahony, Mary

AU - Pierini, Anna

AU - Calzolari, Elisa

AU - Gatt, Miriam

AU - Bakker, Marian

AU - Addor, Marie-Claude

AU - Tucker, David

AU - Klungsoyr, Kari

AU - Latos-Bielenska, Anna

AU - Mejnartowicz, Jan P.

AU - Kallen, Karin

AU - Barisic, Ingeborg

AU - Verellen-Dumoulin, Christine

AU - Doray, Bérénice

AU - Arriola, Larraitz

AU - Wellesley, Diana

AU - Neville, Amanda

AU - De Jong-Van Den Berg, Lolkje T.W.

AU - Dolk, Helen

PY - 2014/10/1

Y1 - 2014/10/1

N2 - Background: Lamotrigine (LTG) is increasingly used during pregnancy. A FDA warning was issued for an association of LTG exposure and increased risk of orofacial clefts (OCs), based on data from the North American Antiepileptic Drug Pregnancy Registry (Holmes, 2006; Holmes et al., 2008). The signal was examined in the European Surveillance of Congenital Anomalies (EUROCAT) antiepileptic-study database (Dolk, 2008). No significantly increased risk of OCs was found relative to other malformations, either for isolated orofacial clefts or for isolated cleft palate. There has been no independent confirmation of increased risk of OCs in relation to LTG from all studies in the literature combined (Dolk et al., 2012). Objectives: To investigate whether first trimester exposure to LTG monotherapy is specifically associated with an increased risk of OCs, using the EUROCAT antiepilepticstudy database including birth years up to 2010. Methods: A population-based case-control study with malformed controls was performed. The updated EUROCAT antiepileptic-study dataset included 226,806 live births, stillbirths, or terminations with malformations among 7.6 million births in 20 European countries from 1995 to 2010, more than twice the population of the original study. Cases were 10,523 nonsyndromic OC registrations, of whom 8,771 were isolated, and 3,789 cleft palate (CP) of whom 2,984 were isolated. Controls were 144,914 non-chromosomal, non-OC registrations. We compared first trimester LTG vs no antiepileptics (non- AED use), for mono and polytherapy. Results: There were 181 LTG exposed (109 mono- and 72 polytherapy) registrations. Thematernal age adjusted odds ratios (ORs) for LTG monotherapy vs non-AED use were 0.84 (95% CI 0.37-1.92) for OC relative to other malformations, 1.01 (95% CI 0.44-2.30) for isolated OC; 1.18 (95% CI 0.38-3.72) for CP, and 1.49 (95% CI 0.47-4.72) for isolated CP. Conclusions: This update does not change the conclusion of the original study: we found no evidence of an increased risk of isolated orofacial clefts relative to other malformations for LTG monotherapy exposure in the first trimester, nor any evidence of an increased risk for isolated cleft palate.

AB - Background: Lamotrigine (LTG) is increasingly used during pregnancy. A FDA warning was issued for an association of LTG exposure and increased risk of orofacial clefts (OCs), based on data from the North American Antiepileptic Drug Pregnancy Registry (Holmes, 2006; Holmes et al., 2008). The signal was examined in the European Surveillance of Congenital Anomalies (EUROCAT) antiepileptic-study database (Dolk, 2008). No significantly increased risk of OCs was found relative to other malformations, either for isolated orofacial clefts or for isolated cleft palate. There has been no independent confirmation of increased risk of OCs in relation to LTG from all studies in the literature combined (Dolk et al., 2012). Objectives: To investigate whether first trimester exposure to LTG monotherapy is specifically associated with an increased risk of OCs, using the EUROCAT antiepilepticstudy database including birth years up to 2010. Methods: A population-based case-control study with malformed controls was performed. The updated EUROCAT antiepileptic-study dataset included 226,806 live births, stillbirths, or terminations with malformations among 7.6 million births in 20 European countries from 1995 to 2010, more than twice the population of the original study. Cases were 10,523 nonsyndromic OC registrations, of whom 8,771 were isolated, and 3,789 cleft palate (CP) of whom 2,984 were isolated. Controls were 144,914 non-chromosomal, non-OC registrations. We compared first trimester LTG vs no antiepileptics (non- AED use), for mono and polytherapy. Results: There were 181 LTG exposed (109 mono- and 72 polytherapy) registrations. Thematernal age adjusted odds ratios (ORs) for LTG monotherapy vs non-AED use were 0.84 (95% CI 0.37-1.92) for OC relative to other malformations, 1.01 (95% CI 0.44-2.30) for isolated OC; 1.18 (95% CI 0.38-3.72) for CP, and 1.49 (95% CI 0.47-4.72) for isolated CP. Conclusions: This update does not change the conclusion of the original study: we found no evidence of an increased risk of isolated orofacial clefts relative to other malformations for LTG monotherapy exposure in the first trimester, nor any evidence of an increased risk for isolated cleft palate.

KW - lamotrigine

KW - anticonvulsive agent

KW - pharmacoepidemiology

KW - risk management

KW - risk

KW - pregnancy

KW - congenital malformation

KW - registration

KW - monotherapy

KW - cleft palate

KW - first trimester pregnancy

KW - exposure

KW - data base

KW - therapy

KW - population

KW - stillbirth

KW - live birth

KW - population based case control study

KW - human

KW - register

KW - food and drug administration

UR - https://onlinelibrary.wiley.com/doi/10.1002/pds.3701

M3 - Meeting Abstract

SN - 1053-8569

VL - 23

SP - 304

JO - Pharmacoepidemiology and Drug Safety

JF - Pharmacoepidemiology and Drug Safety

ER -

Lamotrigine use in pregnancy and risk of orofacial cleft, an update of eurocat lamotrigine study

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