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Book
Year: 2012 Publisher: Bruxelles: UCL,
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Book
Year: 2018 Publisher: Bruxelles: UCL. Faculté de pharmacie et des sciences biomédicales,
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Ce mémoire a pour objectif d'analyser les différentes études cliniques qui ont été réalisées sur une nouvelle formulation orale de la lévodopa : IPX066, et déterminer, au terme d'une discussion, son intérêt et ses perspectives dans l'arsenal thérapeutique de la maladie de Parkinson. Actuellement, la lévodopa demeure le traitement le plus efficace pour contrôler les symptômes moteurs de la maladie de Parkinson. Pratiquement tous les patients en reçoivent au cours de leur maladie. Cependant, cela entraine presque inexorablement des complications motrices (fluctuations motrices et dyskinésies). Dans le but de les limiter, IPX066 a été développé et approuvé par l'EMA (Numient®) et la FDA (Rytary®) en 2015. Cette formulation contient des microbilles de carbidopa-lévodopa à libération immédiate et prolongée permettant une atteinte rapide et un maintien des concentrations plasmatiques thérapeutiques de lévodopa de façon plus continue. Cela entrainerait une stimulation dopaminergique plus constante et donc, une diminution des complications motrices liées à la lévodopa. The purpose of this thesis is to analyze several clinical studies conducted about a new levodopa oral formulation: IPX066 and to identify, following a discussion, its interest and prospects in Parkinson's disease therapeutic arsenal. Levodopa remains currently the most effective treatment managing the motor symptoms of Parkinson’s disease. Almost all patients receive it at some point. However, it leads almost inexorably to motor complications (motor fluctuations and dyskinesia’s). To limit it, IPX066 has been developed and approved by the EMA (Numient®) and FDA (Rytary®) in 2015. This formulation contains immediate and extended release microbeads of carbidopa-levodopa allowing a rapid onset and sustained and more continuous levodopa therapeutic plasma concentrations. lt would lead to more consistent dopaminergic stimulation and thus, a decrease in levodopa-induced motor complications.
Book
Year: 1975 Publisher: Lancaster MTP Press
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Levodopa --- Levodopa --- Parkinsonian Disorders --- therapeutic use --- adverse effects --- drug therapy
Book
Year: 2011 Publisher: Bruxelles: UCL,
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Parkinson Disease --- Levodopa --- Infusions, Parenteral --- Duodenum
Book
Year: 1975 Publisher: Lancaster, Eng.: MTP, Medical and Technical Publishing Co.,
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Levodopa --- Parkinson Disease --- therapeutic use. --- drug therapy.
Film
Year: 1987 Publisher: Leuven KU Leuven. Audiovisuele dienst [prod., real., dist.]
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Circadian Rhythm --- Dystonia --- Levodopa --- therapeutic use
Book
Year: 1989 Publisher: Cleveland (Ohio) : Edgell communications,
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Delayed-action preparations. --- Levodopa. --- Parkinson disease, drug therapy.
Dissertation
Year: 1975 Publisher: Liège : Université de Liège, Institut de psychologie et des sciences de l'éducation (ULg),
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HUMAN --- RORSCHACH TEST --- PARKINSON DISEASE --- LEVODOPA --- DRUG THERAPY --- THERAPEUTIC USE --- HUMAN --- RORSCHACH TEST --- PARKINSON DISEASE --- LEVODOPA --- DRUG THERAPY --- PSYCHOLOGY --- THERAPEUTIC USE
Book
Year: 2009 Publisher: Bruxelles: UCL,
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Tolcapane is an inhibitor of catechol-o-methyltransferase, an enzyme which is responsible for the degradation of dopamine and levopoda in the central and peripheral nervous systems. Its action is both central and peripheral. Tolcapone is administrated in addition to treatment with levodopa and, especially in patients with fluctuations in end-of-dose. It reduces the doses of levodopa and the time spent by patients in “off” periods.
It exists also another catechol-o-methyltransferase inhibitor, entacapone. This molecule has many features in common with tolcapone but its action is only peripheral.
Tolcapone was put on the market in August 1997. However, causing fulminant hepatitis and three deaths, the substance was later withdrawn in December 1998. Today, tolcapone can be prescribed only under a strict liver monitoring and when entacapone is not tolerated or not sufficient. If the treatment is without benefit for eh patient, it will be stopped after three weeks La tolcapone est un inhibiteur de la catéchol-o-méthyltransférase, enzyme responsable de la dégradation de la dopamine et de la lévodopa au niveau central et périphérique. Son action est aussi bien périphérique que central. La tolcapone est administrée en complément d’un traitement à la lévodopa et ce, surtout chez les patients présentant des fluctuations en fin de dose. Elle permet de réduire les doses de cette dernière ainsi que le temps passé par les patients en période « off ».
Il existe également un autre inhibiteur de la catéchol-o-méthyltransférase, l’entacapone. Cette molécule possède nombreuses caractéristiques communes avec la tolcapone mais son action se limite au niveau périphérique.
La tolcapone fut mise sur la marché en août 1997. Cependant, ayant causé des hépatites fulminantes et rois décès consécutifs, la substance dut ensuite retirée en décembre 1998. Aujourd’hui, la tolcapone peut donc à nouveau être prescrite mais seulement dans le cadre d’un monitoring hépatique sévère et lorsque l’entacapone n’est pas tolérée ou ne suffit pas. Si le traitement n’apporte aucun bénéfice pour le patient, il sera stoppé après trois semaines
tolcapone --- Parkinson Disease --- entacapone --- Legislation, Pharmacy --- Pharmaceutical Preparations --- Levodopa --- Antiparkinson Agents
Book
Year: 2020 Publisher: Frontiers Media SA
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This eBook is a collection of articles from a Frontiers Research Topic. Frontiers Research Topics are very popular trademarks of the Frontiers Journals Series: they are collections of at least ten articles, all centered on a particular subject. With their unique mix of varied contributions from Original Research to Review Articles, Frontiers Research Topics unify the most influential researchers, the latest key findings and historical advances in a hot research area! Find out more on how to host your own Frontiers Research Topic or contribute to one as an author by contacting the Frontiers Editorial Office: frontiersin.org/about/contact
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