PARKINSON'S & RASAGILINE
One of the drugs that has emerged as promising and at least somewhat effective in the treatment of Parkinson's disease is known as Rasagiline. This report will explore the neurobiological and psychological implications of the drug as it relates to Parkinson's and in general. The depth and breadth of some of the studies will be discussed as well as how that evidence was found, a general discussion of Rasagiline and its current/future status as a Parkinson's treatment and how all of the above should be taken with a grain of salt given the limitations that exist. There are some great opportunities for future research when it comes to Parkinson's in general and Rasagiline in particular.
Introduction
Parkinson's is a very debilitating and difficult disorder to deal with and treat. Even with the prominence of several major celebrities (e.g. Muhammad Ali, Michael J. Fox, etc.) and increase public awareness in general, the progress on the treatment and a possible cure for Parkinson's has been frustratingly slow. Even so, progress has not been entirely missing as there are drugs like Rasagiline and other options on the market like levodopa. As different drugs and therapies have been tried, there have been some ancillary side effects and other issues. However, as the drugs and the combinations thereof become more robust and complex, the results of these therapies and pharmacological options get better. Even so, it is best to keep a good eye on the neurobiological and psychological impacts of all of the above to ensure the best quality of care and quality of life for the patient.
Method
The author of this report has consulted academic search engines to find peer-reviewed and other academic journal articles that discuss the neurobiological and psychological impacts and outcomes of people on Rasagiline as well as other Parkinson treatments. The latter will be included as a point of comparison as there should be a justification and explanation of when Rasagiline should be used, why it is used and how it tends to be or should be used. Both qualitative and quantitative data shall be used to make the points being driven home in this report. In short, any data that is valid and reliable shall be included as part of the literature review for this study and most journal articles, peer-reviewed in particular, will meet this standard. Of course, the progress and forward movement of Parkinson's treatments and the like is ever-changing so there has been an effort to keep the sources used as recent as possible unless there is a very good reason to include older information and data. Indeed, it is important at times to use the proper points of reference to drive home what is otherwise being asserted in a report like this one.
Results from Recent Studies
One of the main reasons that Rasagiline has come to be a superior option as compared other Parkinson treatments is because of the symptoms of other treatments have caused behavioral issues. One major example of this is impulse control disorders in patients that are taking drugs such as pramipexole and ropinorole. In general, it has been found that dopamine agonists like those two drugs are especially bad about this. A common manifestation of this impulse problem is hyper-sexuality. Further, there is slightly lesser evidence that there is an association between monoamine oxidase type-B inhibitors and the later onset of impulse control disorders. Conversely, Rasagiline is a second-generation MAO-B drug and it tends to induce moderate symptomatic and possibly disease modifying benefits along with good tolerability and a good safety profile in Parkinson's patients. The drug is often effective and well-tolerated when used as a solo therapy (i.e. monotherapy) but significant benefits are also seen when Rasagiline is combined with levodopa (Reyes, Kurako & Galvez-Jimenez, 2014).
When it comes to Rasagiline in particular, there have been extensive studies on how and to what degree the drug has effects on cognitive deficits in Parkinson patients that do not have dementia. Indeed, the work of Hanagasi et al. (2011) was a randomized and double-blind study that looked at this particular subject. As partially noted before, Rasagiline is a selective monoamine oxidase type-B inhibiter that works by enhancing dopaminergic transmission. This is deemed as important and vital to those that treat Parkinson's because dopamine is thought to be involved in certain cognitive processes such as a person's working memory. The Hanagasi study had patients that were receiving stable dopaminergic treatment be given Rasagiline. It was given in the amount of one milligram per day over the course of three months. Others in the group were given a placebo in the same...
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