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A critical appraisal of MAO-B inhibitors in the treatment of Parkinson's disease
release_qou33lceszdbhnqdoffwnseusm
by
Wolfgang H. Jost
Published
in Journal of neural transmission
by Springer Science and Business Media LLC.
2022 Volume 129, Issue 5-6, p723-736
Abstract
<jats:title>Abstract</jats:title>Since the 1980s, the MAO-B inhibitors have gained considerable status in the therapy of the Parkinson's disease. In addition to the symptomatic effect in mono- and combination therapies, a neuroprotective effect has repeatedly been a matter of some discussion, which has unfortunately led to a good many misunderstandings. Due to potential interactions, selegiline has declined in significance in the field. For the MAO-B inhibitor safinamide, recently introduced to the market, an additional inhibition of pathological release of glutamate has been postulated. At present, rasagiline and selegiline are being administered in early therapy as well as in combination with levodopa. Safinamide has been approved only for combination therapy with levodopa when motor fluctuations have occurred. MAO-B inhibitors are a significant therapeutic option for Parkinson's disease, an option which is too often not appreciated properly.
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