Session Information
Date: Saturday, October 6, 2018
Session Title: Parkinson’s Disease: Clinical Trials, Pharmacology And Treatment
Session Time: 1:45pm-3:15pm
Location: Hall 3FG
Objective: Evaluating the efficacy and security starting safinamide treatment with 100 mg/day in PD
Background: Dopaminergic treatment has been useful in PD. Other neurotransmission mechanisms such as glutamate have been implicated in the development of these phenomena. Safinamide has a unique dopaminergic and non-dopaminergic mode of action that includes the enhancement of the dopaminergic transmission through the selective and reversible inhibition of the monoamine-oxidase B enzyme, and the control of the abnormal glutamate release through the state- and use-dependent blockade of the sodium channels which can be appreciated at dose of 100 mg. Safinamide has the potential to improve motor and non-motor symptoms and complications used at 100 mg daily dose since the beginning, such as in the 016 and 018 studies
Methods: Among the population diagnosed with PD in our ambulatory, we identified 60 patients that needed therapeutic adjustment because of worsening of symptoms or complications related to the disease that could benefit from both dopaminergic and glutamatergic mechanisms, being started directly with safinamide 100 mg. We reviewed retrospectively the efficacy and safety of this new therapeutic approach clinical improvement, routine follow up and patient subjective perception of the disease
Results: The evaluation showed good efficacy and safety profile, among the 60 patients identified that have started directly with safinamide 100 mg daily. We found out that 100% (n=60) continued with the treatment showing a very good safety profile. Among them 75% (n=45) showed clinical improvements in non-motor symptoms (mainly in sleep disorders and pain) and motor symptoms and complications (ON time and dyskinesias); 18.33% (n=11) maintained their symptoms and/or complications stable, and only 6.66% (n=4) needed a new medication adjustment (adding opicapone without any safety issue)
Conclusions: Safinamide improved motor and non-motor symptoms and complications without increasing troublesome dyskinesia, maintaining the benefits in the long-term with a significant improvement of patients’ quality of life. These favorable effects may be explained by its modulation of both dopaminergic action and glutamatergic hyperactivity regulation. In our clinical experience starting with a dose of safinamide 100 mg daily is effective and safe, and may offer more benefits than increasing gradually from safinamide 50 mg daily as the patient could benefit from both safinamide actions, dopaminergic and glutamatergic, since the beginning of the treatment.
To cite this abstract in AMA style:
N. Foncea. Efficacy and security starting safinamide treatment with 100 mg/day in PD [abstract]. Mov Disord. 2018; 33 (suppl 2). https://www.mdsabstracts.org/abstract/efficacy-and-security-starting-safinamide-treatment-with-100-mg-day-in-pd/. Accessed October 31, 2024.« Back to 2018 International Congress
MDS Abstracts - https://www.mdsabstracts.org/abstract/efficacy-and-security-starting-safinamide-treatment-with-100-mg-day-in-pd/