Abstracts

This is a Late Breaking abstract

Rationale: Fenfluramine (FFA) is approved in the US for the treatment of seizures associated with Lennox-Gastaut syndrome (LGS) in patients ≥ 2 years of age. LGS-associated disorders exist beyond seizures, including executive function (EF) issues. EF is an important domain for caregivers and families of patients with LGS, who deal with the impact of impairments in regulation of behavior, emotion, and cognition on their daily lives. FFA-treated children and adolescents with LGS in a previous post-hoc analysis showed clinically meaningful improvement in everyday EF. Here, we examine the associations between placebo and two FFA dosages and clinically meaningful changes on everyday EF over 14 weeks from a phase 3 trial in adults with LGS.

Methods: Everyday EF was assessed by caregivers with the Behavior Rating Inventory of Executive Function^®—Adult Version (BRIEF^®-A) indexes/composite and scales. Clinically meaningful improvement and worsening were defined using Reliable Change Index (RCI) ≥ 90% and ≥ 80% certainty, respectively. Associations between treatment groups (placebo, FFA 0.2 mg/kg/day, and FFA 0.7 mg/kg/day) and the likelihood of clinically meaningful change were calculated using cross-tabulations and Somers’ d (p≤0.05); when significant, two-sided Fisher’s Exact pairwise comparisons were performed (p≤0.05).

Results: Data were analyzed for 57 adults with LGS aged 19-35 years (placebo, n=23; FFA 0.2mg/kg/day, n=18; FFA 0.7mg/kg/day, n=16). All described associations met the a priori threshold (p≤0.05). There were positive associations between treatment groups and the likelihood of clinically meaningful improvement in the two indexes (Behavior Regulation Index, BRI; Metacognition Index, MI) and the global executive composite (GEC; Figure 1). Higher-dose FFA showed a greater likelihood of clinically meaningful improvement than placebo in MI. There were positive associations between the treatment groups and the likelihood of clinically meaningful improvement in three of four scales that comprise BRI (Inhibit, Shift, Self-Monitor) and three of five scales that comprise MI (Initiate, Task Monitor, and Organization of Materials; Figure 2). Higher-dose FFA showed a greater likelihood of clinically meaningful improvement than placebo in the Inhibit, Initiate, Task Monitor, and Organization of Materials scales. Lower-dose FFA showed a greater likelihood of clinically meaningful improvement than placebo in the Shift scale. There were no significant associations between treatment groups and the likelihood of clinically meaningful worsening.

Conclusions: FFA was associated with clinically meaningful improvements in everyday EF in adults with LGS over a relatively short treatment period. Higher-dose FFA showed a greater likelihood of clinically meaningful improvement in everyday cognitive regulation, driven by improvements in initiating, task monitoring, and organizing materials and environment. These data suggest that treatment with FFA initiated in adulthood also confers benefits in everyday EF.

Funding: UCB