Type of paper:Â | Research proposal |
Categories:Â | Medicine Case study Mental disorder |
Pages: | 3 |
Wordcount: | 583 words |
This study is carried out to show that the most common atypical Parkinsonian syndrome for Therapeutic study is Progressive Supranuclear Palsy. Clinical findings associated with this syndrome include early postural falls and instability, early dysphagia and dysarthria, deficits of frontal cognitive, supranuclear gaze palsy that is verticle and akinetic-rigid parkinsonism that is symmetric. Mostly used therapeutic approaches are done on open trails, studies of placebo and double-blind that are small with an expectation that future trials will involve double-blind that is large, design under control and placebo. The diseases under experiment that turn out to modify the Therapeutic trial involves the following: glutamatergic and glycogen synthase kinase inhibitors and stabilizers that are microtubule. Additional inhibitors like Rho kinase, calpain, microglial and CDK5 and, anti-inflammatories and Tau antibodies are being translated into this specific trial with the reason of their positive effects in the models of tauopathies in transgenic animals (Shoeibi & Litvan, 2017).
Hypothesis
In the Therapeutic study, there is a high expectation of a dreadful impact on the systems of health with the reason of progression of Alzheimer's disease (AD) and the in-effective therapy measures. With the many trials to come up with strategies for handling this disease, a certain area of concern has been identified as sirtuins. By definition, Sirtuins (SIRTs) are conserved enzymes that are evolutionary with an activity called deacetylase that is majorly involved in a plethora of metabolic functions. There are generally seven sirtuins (SIRT1-7) inanimate beings. There is an increased possibility of other discoveries for strategies of handling neuroprotective therapeutic for this disease due to the recent discovery of information on molecular targets of SIRT1, SIRT2, and SIRT3.an advantage of this sirtuins is that they are a consummate small drug target for inhibitors and activators (Polito et al.2017).
Some other characteristic of this disease is Inflammation and neurodegenerative disorders. It is easy to resolve inflammation and the tissue returned to homeostasis. Disturbance of activities of pro-resolving leads to inflammation that is chronic hence resulting in a disease. Correspondingly, chronic inflammation in the Alzheimer's disease brain may result from resolution failure with evidence of a diminution in the levels of specialized pro-resolving lipid mediators (SPMs. Stimulation of pro-resolving activities furnish neuroprotection change a proinflammatory phenotype toward a homeostatic phenotype. Consequently, the specialized pro-resolving lipid mediators' action by inhibition of inflammation by an increment in the glial uptake and a reduction in production is important for breaking the circle of reciprocal stimulation of inflammation and amyloidosis ( Polito et al.2017).
Therapeutic approach
The potential therapeutic approach in the process of managing the patients so that their quality of life and health can be bettered. Pathophysiology of this disease is highly required, though mechanisms in pathophysiology TDP-43 reveal a confident outlook in the recognition of novel therapies. Furthermore, the issue of multidisciplinary specialized clinics has led to an increment in the survival and quality of life among patients (Shoeib & Litvan, 2017).
References
Mathis, S., Couratier, P., Julian, A., Vallat, J. M., Corcia, P., & Le Masson, G. (2017). Management and therapeutic perspectives in amyotrophic lateral sclerosis. Expert review of neurotherapeutics, 17(3), 263-276. https://www.tandfonline.com/doi/abs/10.1080/14737175.2016.1227705
Polito, L., Biella, G., & Albani, D. (2017). Sirtuin modulation as novel neuroprotective strategy for Alzheimer's disease. In Neuroprotection in Alzheimer's Disease (pp. 149-173). Academic Press. https://www.sciencedirect.com/science/article/pii/B9780128036907000090
Shoeibi, A., & Litvan, I. (2017). Therapeutic options for Progressive Supranuclear Palsy including investigational drugs. Expert Opinion on Orphan Drugs, 5(7), 575-587. https://www.tandfonline.com/doi/full/10.1080/21678707.2017.1335596?scroll=top&needAccess=true
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Essay Sample. Progressive Supranuclear Palsy. (2023, May 23). Retrieved from https://speedypaper.com/essays/progressive-supranuclear-palsy
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