Hyperandrogenism, ovulatory dysfunction, and polycystic ovary syndrome with valproate versus lamotrigine

MJ Morrell, FJ Hayes, PM Sluss… - Annals of Neurology …, 2008 - Wiley Online Library
MJ Morrell, FJ Hayes, PM Sluss, JM Adams, M Bhatt, C Ozkara, CR Warnock MS, J Isojärvi
Annals of Neurology: Official Journal of the American Neurological …, 2008Wiley Online Library
Objective To evaluate development of components of polycystic ovary syndrome (PCOS)
and PCOS in women with epilepsy initiating valproate or lamotrigine therapy. Methods
Female individuals with epilepsy and regular menstrual cycles were eligible for this
prospective study. Participants were randomized to 12 months of valproate (n= 225) or
lamotrigine (n= 222) therapy. Serum androgen levels were measured every 3 months.
Urinary pregnanediol glucuronide levels were measured weekly for two 3‐month periods …
Objective
To evaluate development of components of polycystic ovary syndrome (PCOS) and PCOS in women with epilepsy initiating valproate or lamotrigine therapy.
Methods
Female individuals with epilepsy and regular menstrual cycles were eligible for this prospective study. Participants were randomized to 12 months of valproate (n = 225) or lamotrigine (n = 222) therapy. Serum androgen levels were measured every 3 months. Urinary pregnanediol glucuronide levels were measured weekly for two 3‐month periods. The primary end point was development of PCOS components (ie, hyperandrogenism or ovulatory dysfunction). A post hoc analysis was conducted in women more than 2 years after menarche (177 lamotrigine, (HA) 186 valproate) to exclude OD the confounding effect of puberty.
Results
More women in the valproate group than the lamotrigine group developed (OD) in the prospective (54% valproate, 38% lamotrigine; p = 0.010) and the post hoc (HA) analyses (36% valproate, 23% lamotrigine; p = 0.007). More women in the valproate group than the lamotrigine group developed PCOS (9 vs 2%; p = 0.007). Development of HA was more frequent with OD valproate than lamotrigine among those initiating treatment at age younger than 26 years (44% valproate, 23% lamotrigine; p = 0.002) but was similar if treatment was started at age 26 years or older (24% valproate, 22% lamotrigine).
Interpretation
Development of HA occurred more frequently with valproate than lamotrigine, especially if medication was started at age younger than 26 years. Ann Neurol 2008;64:200–211
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