Safinamide: an add-on treatment for managing Parkinson’s disease

Safinamide: an add-on treatment for managing Parkinson’s disease

Thomas Müller Department of Neurology, St. Joseph Hospital Berlin-Weißensee, Berlin, Germany Abstract: Heterogeneous expression of neurotransmitter deficits results from onset and progression of Parkinson’s disease. Intervals, characterized by reappearance of motor and a...

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Main Author: Müller T
Format: Article
Language:English
Published: Dove Medical Press 2018-04-01
Series:Clinical Pharmacology : Advances and Applications
Subjects:
Safinamide
MAO-B inhibition
abnormal glutamate release inhibition
Parkinson’s disease
dopamine substitution
glutamate
Online Access:https://www.dovepress.com/safinamide-an-add-on-treatment-for-managing-parkinsons-disease-peer-reviewed-article-CPAA
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spelling doaj-8c06556cab854d36b3a3812b7e6f2ccc2020-11-24T21:24:43ZengDove Medical PressClinical Pharmacology : Advances and Applications1179-14382018-04-01Volume 10314137593Safinamide: an add-on treatment for managing Parkinson’s diseaseMüller TThomas Müller Department of Neurology, St. Joseph Hospital Berlin-Weißensee, Berlin, Germany Abstract: Heterogeneous expression of neurotransmitter deficits results from onset and progression of Parkinson’s disease. Intervals, characterized by reappearance of motor and associated certain nonmotor symptoms, determine the end of good tolerability and efficacy of oral levodopa therapy. These “OFF” states result from levodopa pharmacokinetics and disease progression-related deterioration of the central buffering capacity for fluctuations of dopamine levels. This review discusses safinamide as an add-on therapeutic agent in orally levodopa-treated patients with “OFF” phenomena. Safinamide provided beneficial effects on “OFF” symptoms in pivotal trials with doses of 50 or 100 mg once daily. Safinamide reversibly inhibits monoamine oxidase B and declines abnormal glutamate release by modulation of potassium- and sodium ion channels. An ideal candidate for combination with safinamide is opicapone. This inhibitor of peripheral catechol-O-methyltransferase supports continuous brain delivery of levodopa and, thus, the continuous dopaminergic stimulation concept. Both compounds with their once-daily application and good tolerability may complement each other by reduction of necessary oral levodopa intakes and “OFF” times. Thus, a promising, future option will be combination of safinamide and opicapone in one formulation. It will reduce adherence issues and may complement levodopa treatment. It will probably cause less nausea and edema than a dopamine agonist/levodopa regimen. Keywords: safinamide, MAO-B inhibition, abnormal glutamate release inhibition, Parkinson’s disease, dopamine substitution, glutamatehttps://www.dovepress.com/safinamide-an-add-on-treatment-for-managing-parkinsons-disease-peer-reviewed-article-CPAASafinamideMAO-B inhibitionabnormal glutamate release inhibitionParkinson’s diseasedopamine substitutionglutamate
collection DOAJ
language English
format Article
sources DOAJ
author Müller T
spellingShingle Müller T
Safinamide: an add-on treatment for managing Parkinson’s disease
Clinical Pharmacology : Advances and Applications
Safinamide
MAO-B inhibition
abnormal glutamate release inhibition
Parkinson’s disease
dopamine substitution
glutamate
author_facet Müller T
author_sort Müller T
title Safinamide: an add-on treatment for managing Parkinson’s disease
title_short Safinamide: an add-on treatment for managing Parkinson’s disease
title_full Safinamide: an add-on treatment for managing Parkinson’s disease
title_fullStr Safinamide: an add-on treatment for managing Parkinson’s disease
title_full_unstemmed Safinamide: an add-on treatment for managing Parkinson’s disease
title_sort safinamide: an add-on treatment for managing parkinson’s disease
publisher Dove Medical Press
series Clinical Pharmacology : Advances and Applications
issn 1179-1438
publishDate 2018-04-01
description Thomas Müller Department of Neurology, St. Joseph Hospital Berlin-Weißensee, Berlin, Germany Abstract: Heterogeneous expression of neurotransmitter deficits results from onset and progression of Parkinson’s disease. Intervals, characterized by reappearance of motor and associated certain nonmotor symptoms, determine the end of good tolerability and efficacy of oral levodopa therapy. These “OFF” states result from levodopa pharmacokinetics and disease progression-related deterioration of the central buffering capacity for fluctuations of dopamine levels. This review discusses safinamide as an add-on therapeutic agent in orally levodopa-treated patients with “OFF” phenomena. Safinamide provided beneficial effects on “OFF” symptoms in pivotal trials with doses of 50 or 100 mg once daily. Safinamide reversibly inhibits monoamine oxidase B and declines abnormal glutamate release by modulation of potassium- and sodium ion channels. An ideal candidate for combination with safinamide is opicapone. This inhibitor of peripheral catechol-O-methyltransferase supports continuous brain delivery of levodopa and, thus, the continuous dopaminergic stimulation concept. Both compounds with their once-daily application and good tolerability may complement each other by reduction of necessary oral levodopa intakes and “OFF” times. Thus, a promising, future option will be combination of safinamide and opicapone in one formulation. It will reduce adherence issues and may complement levodopa treatment. It will probably cause less nausea and edema than a dopamine agonist/levodopa regimen. Keywords: safinamide, MAO-B inhibition, abnormal glutamate release inhibition, Parkinson’s disease, dopamine substitution, glutamate
topic Safinamide
MAO-B inhibition
abnormal glutamate release inhibition
Parkinson’s disease
dopamine substitution
glutamate
url https://www.dovepress.com/safinamide-an-add-on-treatment-for-managing-parkinsons-disease-peer-reviewed-article-CPAA
work_keys_str_mv AT mullert safinamideanaddontreatmentformanagingparkinsonrsquosdisease
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