Home
Username:  
Password:
Forgot Password  |  Login Help
  Free LiveMed Journal subscription

|

Advertise

|

Feedback

|

About Us

|

Contact Us
HomeHome
LMJ by SpecialistsLMJ by Specialty
Upcoming JournalsUpcoming Journals
ArchivesJournal Archives
CME CoursesCME Courses
Be a SpeakerBe a Speaker
Email AlertsEmail Alerts
PodcastsPodcasts
Search WebSearch Web
 

Powered By
 
IndentAdPlayer2
  Journal Detail  
  Journal
   

Playback video/audio of archived journal session



Related Documents (2)
Discussion Forum (1)

In utero antiepileptic drug exposure: Fetal death and malformations
K. J. Meador, MD, G. A. Baker, PhD, R. H. Finnell, PhD, L. A. Kalayjian, MD, J. D. Liporace, MD, D. W. Loring, PhD, G. Mawer, MD, P. B. Pennell, MD, J. C. Smith, MD, M. C. Wolff, PhD for the NEAD
Presenter(s): Kimford Meador, MD. University of Florida, Melvin Greer Professor of Neurology
Specialty: Neurology

Date: Wed, Nov 29, 2006 at 12:30 PM
Short Abstract:

BACKGROUND: Pregnancy outcomes following in utero exposure to antiepileptic drugs (AEDs) are uncertain, limiting an evidenced-based approach. OBJECTIVE: To determine if fetal outcomes vary as a function of different in utero AED exposures. METHODS: This ongoing prospective observational study across 25 epilepsy centers in the USA and UK enrolled pregnant women with epilepsy from October 1999 to February 2004 to determine if differential long-term cognitive and behavioral neurodevelopmental effects exist across the four most commonly used AEDs. This initial report focuses on the incidence of serious adverse outcomes including major congenital malformations (which could be attributable to AEDs) or fetal death. A total of 333 mother/child pairs were analyzed for monotherapy exposures: carbamazepine (n = 110), lamotrigine (n = 98), phenytoin (n = 56), and valproate (n = 69). RESULTS: Response frequencies of pregnancies resulting in serious adverse outcomes for each AED were as follows: carbamazepine 8.2%, lamotrigine 1.0%, phenytoin 10.7%, and valproate 20.3%. Distribution of serious adverse outcomes differed significantly across AEDs and was not explained by factors other than in utero AED exposure. Valproate exhibited a dose-dependent effect. CONCLUSIONS: More adverse outcomes were observed in pregnancies with in utero valproate exposure vs the other antiepileptic drugs (AEDs). These results combined with several recent studies provide strong evidence that valproate poses the highest risk to the fetus. For women who fail other AEDs and require valproate, the dose should be limited if possible.
 
     

DISCLAIMER: The content of this Website is not influenced by sponsors. The site is designed primarily for use by qualified physicians and other medical professionals. The information contained herein should NOT be used as a substitute for the advice of an appropriately qualified and licensed physician or other health care provider. The information provided here is for educational and informational purposes only. In no way should it be considered as offering medical advice. Please check with a physician if you suspect you are ill.
Terms and Conditions | Privacy Policy
LiveMed Journal - Version 1.0 © LiveMed Journal 2006