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Clinical Trial Summary

This purpose of this study is to explore the relationships of exercise on inflammation in the body in older adults and people with Parkinson's disease (PD). This is important research for older adults and but is especially important for people with PD because neuroinflammation is the main pathological mechanism that is responsible for neuron cell death in this neurodegenerative disease. As PD is a progressive disease, halting or slowing the degeneration is an important research target. Halting or slowing the disease progress is known as neuroprotection. Exercise is an attractive therapeutic treatment for people with PD as it has a lot of multi-systemic benefits but also there is a lot of evidence to suggest that it helps improve symptoms and slow the progression of the disease. Exercise has been theorized to decreased inflammation and, therefore, has a lot of promise as a neuroprotective agent in slowing or halting the degeneration in PD. Unfortunately, there is not a lot of research that has looked into the effect of exercise on the biological processes of inflammation. Thus, the purpose of this study is to investigate the biological evidence that underlies the positive effect of exercise in people with PD.


Clinical Trial Description

Parkinson's disease (PD) is the second most common neurodegenerative disease, affecting an estimated 4 million individuals and 1% of those over the age of 60. The pathologic hallmark of PD are Lewy bodies in neurons and these inclusion bodies are largely made up of misfolded α-synuclein. These α-synuclein inclusion bodies cause mitochondrial respiratory dysfunction which results in reactive oxygen species causing oxidative stress; this, in turn, leads to more aggregation of α-synuclein and a vicious cycle ensues. Ultimately, this vicious cycle results in dopaminergic neuron cell death causing a decrease in dopamine in the nigrostriatal pathway. Mitochondrial dysfunction and subsequent oxidative stress are also caused by environmental toxins (e.g., trichloroethylene, paraquat) and neuroinflammation, both of which are theorized to play a prominent role in PD pathology. Because of this, neuroprotective strategies in PD have focused on limiting exposure to environmental toxins and, more importantly, decreasing pro-inflammatory mechanisms. Evidence has been accumulating that exercise improves symptoms and quality of life and is neuroprotective in PD. In one meta-analysis, they found that regular exercise delays the progression of PD motor symptoms, mobility, and balance deterioration. Another meta-analysis reported a reduced risk for developing PD in the pre-clinical phase for those performing moderate to vigorous exercise. Another meta-analysis showed a 40% risk reduction in developing PD for people regularly performing moderate to vigorous activity aged 35-39 or within the previous ten years. Based on these findings, it can be reasonably deduced that moderate to vigorous exercise prior to PD diagnosis is neuroprotective. Moreover, exercise may also slow the progression of degeneration after PD diagnosis. A prominent theory underlying neuroprotection in PD is that exercise may mitigate the pro-inflammatory milieu thereby protecting and slowing the progressive loss of dopaminergic neurons. Various chemical mediators, antioxidant agents, and cytokines have been shown to play a role in the development, progression, and severity of PD, including interleukin 6 (IL-6) and 10 (IL-10), tumor necrosis factor (TNF), and the interferon gamma family (IFNγ). Some of these chemicals are anti-inflammatory and some are pro-inflammatory. While these are some of the most commonly studied cytokines, there are many others that are understudied in PD and they may also contribute to the internal state of inflammation in PD. Therefore, it is important to examine the collective blend of these cytokines and chemokines to understand the inflammatory milieu in PD as a result of acute and chronic exercise. While regular exercise may be neuroprotective in PD by reducing oxidative stress, the release of antioxidant enzymes via exercise (superoxide dismutase (SOD), glutathione peroxidase, catalase) may also contribute to an overall decrease in the state of inflammation in PD. Another group of compounds theorized to play a role in the mitigation of PD progression are the neurotrophins (e.g., brain-derived neurotrophic factor (BDNF), vascular endothelial growth factor (VEGF), glial cell line-derived neurotrophic factor (GDNF)). All three of the aforementioned neurotrophins are activity-dependent meaning they increase as a result of exercise. GDNF and BDNF have received the most attention and are theorized to aid in neuroregeneration and neuroprotection in PD by protecting dopaminergic neurons. There are decreased levels of BDNF in the dopaminergic nigrostriatal pathways in people with PD (PwP). A reduction in the bioavailability of dopamine compounded by a decrease in BDNF has been shown to be associated with PD signs (movement dysfunction, resting tremor, and bradykinesia). Additionally, BDNF may also be related to an anti-inflammatory milieu in PD thereby highlighting the need to investigate the cytokines and neurotrophins together. Lastly, VEGF may indirectly impact neuroprotection in PD by improving blood supply (angiogenesis) and synaptic activity. Thus, there are three possible mechanisms that are theorized to underlie the disease modifying effects of exercise in PD: decreasing the inflammatory milieu via cytokines, decreasing the inflammatory milieu via antioxidant enzymes, and improved neuroprotection of neurons via neurotrophins. Currently, it is not understood if one of these methods predominates or if it is the combination of these mechanisms that underlie neuroprotection. Theoretically, all three mechanisms may slow the progression of PD by breaking up the vicious cycle of α-synuclein aggregation, mitochondrial toxicity, and oxidative stress. These purported mechanisms warrant further research attention. Importantly, there are no studies to our knowledge that have looked at all three mechanisms together in one study. Since there are interrelationships among the three mechanisms it makes sense to explore these in more detail. Importantly, it is not known how these mechanisms respond to different doses of exercise. Therefore, this study will examine the relationship of exercise dose to these mechanisms to gain greater insight into neuroprotection in PD. The following are the specific aims of this study: Primary Aim 1 (exercise and inflammatory milieu): To determine if there is an association between current exercise/physical activity habits and levels of cytokines, antioxidant enzymes, and neurotrophins after controlling for PD progression, age, sex, body mass index, inflammatory-related genotypes, and number of comorbidities. Hypothesis 1: PwP who are regular exercisers will have less inflammation (more anti-inflammatory cytokines and/or fewer pro-inflammatory cytokines) and higher levels of antioxidant enzymes and neurotrophins compared to those who are not regular exercisers. Primary Aim 2 (inflammatory milieu comparison to controls): To determine if there is a difference between PwP and healthy controls on levels of cytokines, antioxidant enzymes, and neurotrophins after controlling for age, sex, body mass index, inflammatory-related genotypes, and number of comorbidities. Hypothesis 2: PwP will have higher levels of more inflammation and lower levels of antioxidant enzymes and neurotrophins compared to healthy, age-matched controls. Primary Aim 3 (exercise dose and biomarkers): To determine if there is a difference before and after 30 minutes of aerobic exercise at 60-70% and 75-85% of the estimated maximum heart rate (EMHR) in PwP and healthy, age-matched controls. Hypothesis 3: There will be an interaction (e.g., different slope of pro- and anti-inflammatory cytokines) between prior level of exercise (regular exercisers versus non-regular exercisers using the Centers for Disease Control (CDC) 150 minutes of regular exercise per week), exercise intensity (60-70% and 75-85% of EMHR), and status (PwP and control) on the change in inflammation, antioxidant enzymes, and neurotrophins. Primary Aim 4 (biomarkers in PD): To determine which of an array of biomarkers is most associated with PD compared to controls and which of those biomarkers is the most associated with exercise and PD progression (MDS-UPDRS score divided by years since diagnosis). Hypothesis 4: Among an array of markers, the investigators expect to see the difference between PwP and controls for the following: cytokines, antioxidant enzymes, and neurotrophins. Hypothesis 5: Among an array of markers, the investigators expect to see the greatest changes before and after higher intensity exercise in PwP in the following: cytokines, antioxidant enzymes, and neurotrophins. ;


Study Design


Related Conditions & MeSH terms


NCT number NCT05854524
Study type Interventional
Source University of Nevada, Las Vegas
Contact Merrill Landers, DPT, PhD
Phone 17028951377
Email merrill.landers@unlv.edu
Status Not yet recruiting
Phase N/A
Start date February 1, 2024
Completion date December 30, 2026

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