Sleep Apnea Clinical Trial
Official title:
Spatial and Temporal Response of Cerebrovascular Response in OSA
Obstructive sleep apnea (OSA) is a prevalent sleep breathing disorder in the general
population in which recurrent collapse of the upper airway occurs during sleep. OSA is more
prevalent in subjects with stroke and is associated with a 3 fold increased risk of stroke.
This makes it a serious public health problem. Approximately 50% of subjects with OSA are
asymptomatic and are often only detected following investigation for the cause of heart
disease or a stroke. In subjects who are treated for OSA many are intolerant or poorly
compliant with treatment. Therefore, the identification of those subjects with OSA most at
risk of adverse consequences such as stroke is important, so that treatment compliance can
be improved.
Therfore, the investigators want to determine if compared to subjects without OSA, subjects
with OSA have evidence of increased stroke risk by assessment of changes in cerebral blood
flow (cerebrovascular reactivity) as measured on Doppler ultrasound of the middle cerebral
artery (TCD) and blood oxygen level-dependent magnetic resonance imaging of patterns of
cerebral blood flow (BOLD MRI) to two stimuli. These stimuli include increased carbon
dioxide concentrations (causes increased cerebral blood flow) and reduced oxygen
concentrations (causing decreased cerebral blood flow). In order to deliver these stimuli
the investigators will use a special machine (RespiractTM) which allows for the precise
control of carbon dioxide and oxygen concentrations in the lungs and blood. The precise
control of carbon dioxide and oxygen in conjunction with BOLD MRI has enabled the production
of detailed maps of the brain that identify areas of healthy and abnormal blood supply.
OSA is associated with increased risk of cardiovascular and cerebrovascular disease compared to the general population. The mechanism for the increased stroke risk in OSA is unknown. However, the constellation of adverse pathophysiological consequences, including intermittent hypoxia and carbon-dioxide retention as a result of OSA may be detrimental to CVR and predispose the brain to ischemia. Previous studies in OSA subjects have measured CVR only using TCD. Therefore, our study will examine CVR by two methods (TCD and BOLD-MRI) with reliable and reproducible hypercapnia and independent control of oxygen saturation (RespiractTM). Patterns seen on CVR may eventually allow the identification of OSA patients who will be at greatest risk for stroke and will therefore, require aggressive risk reduction and/or treatment irrespective of symptoms. ;
Observational Model: Cohort, Time Perspective: Prospective
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