4.6 Article

Effect of clinical features on antiseizure medication doses in patients with newly diagnosed epilepsy

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FRONTIERS IN NEUROLOGY
卷 14, 期 -, 页码 -

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FRONTIERS MEDIA SA
DOI: 10.3389/fneur.2023.1159339

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antiseizure medication; newly diagnosed epilepsy; seizure freedom; treatment outcomes; oxcarbazepine; valproic acid; carbamazepine

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This study evaluates the impact of various clinical features on the dosage of anti-seizure medication in new-onset epilepsy patients aged 16 years and above. The findings indicate that there are dosage differences in oxcarbazepine among different age groups; men require higher doses of valproic acid compared to women; carbamazepine dosage is influenced by certain seizure types. These results provide insights for individualizing initial target dosages based on clinical characteristics.
ObjectiveWe evaluate the effect of distinct clinical features on anti-seizure medication (ASM) doses in seizure-free and not seizure-free patients aged & GE;16 years with new-onset epilepsy. Materials and methodsThis study included 459 patients with a validated diagnosis of epilepsy. The most prescribed ASMs were oxcarbazepine (OXC; n = 307), followed by valproic acid (VPA; n = 115), carbamazepine (CBZ; n = 81), and lamotrigine (LTG; n = 67). The seizure freedom rate with their first or subsequent ASM was 88.0%. A retrospective analysis of patient records was performed to determine any association between doses of ASMs and patient characteristics. ResultsThe median OXC dose in seizure-free patients aged >60 years was 600 mg compared to 900 mg in younger patients. When controlling for age but not in an unadjusted model, the median dose of OXC was lower (300 mg, p = 0.018) for seizure-free patients compared to non-seizure-free patients, and the median dose of OXC was also 300 mg lower among older patients aged >60 years (p < 0.001). The median OXC doses for men aged & LE;60 years were 300 mg higher than for women aged >60 years (900 mg vs. 600 mg, p = 0.021). The median dose of VPA was 400 mg higher in men than in women (p < 0.001) and 400 mg higher in not seizure-free patients compared to seizure-free patients only when adjusting for sex (p < 0.001). Higher median doses for CBZ were registered with FAS compared with FBTCS (difference in median doses of 200 mg; p = 0.017). ConclusionSignificant OXC dose differences were detected between age groups, whereas VPA dosing was different in men and women. Moreover, CBZ doses were dependent on some seizure types. These data allow for the individualization of the initial target dosing based on key clinical characteristics.

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