Epilepsy Clinical Trial
Official title:
Lamotrigine Pregnancy Registry (LAM05)
Antiepileptic drugs (AEDs) are not indicated for use in pregnancy. However, women with epilepsy, and other approved indications including bipolar disorder, may require or be unintentionally exposed to AEDs during pregnancy. Prior to an AED being marketed there are few data available on drug safety in pregnancy: data from animal models may not translate directly to humans and pregnant women are routinely excluded from clinical trials. The International Lamotrigine Pregnancy Registry was established by GlaxoSmithKline (GSK) in 1992 to monitor the safety of lamotrigine during pregnancy.
The International Lamotrigine Pregnancy Registry aims to assess whether there is a
substantial increase in the risk of major congenital malformations (MCMs) following in utero
exposure to lamotrigine. Exposure during the first trimester is of primary interest as this
represents the period of organogenesis. The Registry is a primarily prospective enrolment
and follow-up study. Patients exposed to lamotrigine during pregnancy are enrolled, on a
voluntary basis, by their healthcare provider. Enrolment is encouraged early in pregnancy
and if possible prior to any prenatal testing. The healthcare provider provides initial
information concerning patient demographics; details of the pregnancy including the
estimated delivery date and results of any prenatal testing; and the timing, duration and
dosage of lamotrigine exposure in pregnancy. The registry accepts exposure reports from
anywhere in the world. Within the United States (US) the healthcare provider can contact the
registry using a toll free number. Outside of the US enrolments are made through the
GlaxoSmithKline local operating company.
Close to the estimated date of delivery the healthcare provider is contacted by the Registry
to provide follow up information concerning the pregnancy outcome (live or still birth,
spontaneous or induced abortion), the presence or absence of a MCM, and the history of
exposure to lamotrigine as well other antiepileptics and antipsychotics during pregnancy. Up
to six attempts are made to contact the healthcare provider to obtain pregnancy outcome
information. After six attempts, the record is closed as lost to follow up. Pregnancy
outcomes are classified as outcomes with MCMs, outcomes without MCMs and spontaneous
abortions. The outcomes with and without MCMs are further classified as live births,
stillbirths/fetal deaths and induced abortions. Spontaneous abortions are reported
separately due to potential for inconsistent identification of malformations in that
situation.
It is beyond the scope of the Registry to consistently access pediatric evaluations and
medical records. For this reason the main outcome is restricted to major congenital
malformations that are external and recognizable in the delivery room or shortly after
birth. To provide consistency, reported congenital malformations are classified as major or
minor according to criteria used by the Centers for Disease Control and Prevention (CDC)'s
Metropolitan Atlanta Congenital Defects Program (MACDP). All malformation reports are
reviewed and classified by a paediatrician from the CDC and further information is requested
as necessary.
Analyses are restricted to prospectively enrolled pregnancies (enrolment prior to knowledge
of the birth outcome). Retrospectively enrolled pregnancies are reviewed for patterns of
defect types, but are not included in formal analyses as retrospective reporting can be
biased towards more unusual and severe outcomes and are less likely to be representative of
the general population experience. The proportion of infants with MCMs among prospectively
reported exposures is calculated as: the total number of outcomes with major birth defects
(number of outcomes with major birth defects + the number of live births without defects).
Chromosomal malformations are reported descriptively, but are not included in the numerator
as it is very unlikely that they are associated with drug exposure during pregnancy. All
spontaneous pregnancy losses, as well as induced abortions and fetal deaths without reported
defects, are excluded from the denominator due to the potential for inconsistent
identification of malformations in those situations. The 95% confidence intervals (CIs) for
risk estimates are calculated using exact methods based on the binomial distribution.
Analyses are stratified according to trimester of exposure (with the second trimester
starting at week 14 and the third trimester at week 28 of gestation) and by exposure group
(lamotrigine monotherapy, lamotrigine polytherapy including valproate and lamotrigine
polytherapy without valproate).
The registry does not have an internal comparator group, but descriptive comparisons are
made with MCM rates from general population studies in the literature and from other ongoing
AED pregnancy registries. Prospective reports are also reviewed to detect any unusual
patterns of malformation types that may warrant further investigation. The data from the
International Lamotrigine Pregnancy Registry are reviewed, and conclusions developed, by an
independent scientific advisory committee. A semi-annual interim report summarizing
aggregate data is provided to disseminate information on a regular basis.
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