Mild Intermittent Hypoxia and Its Multipronged Effect on Sleep Apnea



Status:Recruiting
Conditions:Insomnia Sleep Studies, Pulmonary, Pulmonary
Therapuetic Areas:Psychiatry / Psychology, Pulmonary / Respiratory Diseases
Healthy:No
Age Range:18 - 60
Updated:11/18/2018
Start Date:November 2018
End Date:October 2020
Contact:Jason H Mateika, Ph.D.
Email:am1819@wayne.edu
Phone:313-576-4481

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Mild Intermittent Hypoxia and CPAP: A Multi-pronged Approach to Treat Sleep Apnea in Intact and Spinal Cord Injured Humans

Mild intermittent hypoxia (IH) initiates sustained increases in chest wall and upper airway
muscle activity in humans. This sustained increase is a form of respiratory plasticity known
as long-term facilitation (LTF). Repeated daily exposure to mild IH that leads to the
initiation of LTF of upper airway muscle activity could lead to increased stability of the
upper airway. In line with PI's laboratory's mandate to develop innovative therapies to treat
sleep apnea, this increased stability could ultimately reduce the continuous positive airway
pressure (CPAP) required to treat obstructive sleep apnea (OSA) and improve compliance with
this gold standard treatment. Improved compliance could ultimately serve to mitigate those
comorbidities linked to sleep apnea. Moreover, in addition to improving CPAP compliance
numerous studies indicate that mild IH has many direct beneficial effects on cardiovascular,
neurocognitive and metabolic function. Thus, mild IH could serve as a multipronged
therapeutic approach to treat sleep apnea. In accordance with this postulation, our proposal
will determine if repeated daily exposure to mild IH serves as an adjunct therapy coupled
with CPAP to mitigate associated co-morbidities via its direct effects on a variety of
cardiovascular, metabolic and neurocognitive measures and indirectly by improving CPAP
compliance. Modifications in autonomic (i.e. sympathetic nervous system activity) and
cardiovascular (i.e. blood pressure) function will be the primary outcome measures coupled to
secondary measures of metabolic and neurocognitive outcomes.

The dogma over the past 3 decades, particularly in the field of sleep medicine, has been that
intermittent hypoxia (IH) is a detrimental stimulus that leads to a number of co‐morbidities
including autonomic (e.g. increased sympathetic nervous system activity), cardiovascular
(e.g. hypertension, atherosclerosis, arterial fibrillation), cognitive (e.g. loss of gray
matter, neural injury and impaired neural function coupled to sleepiness) and metabolic
dysfunction (dyslipidemia, hyperglycemia, insulin resistance). This belief was based
principally on animal studies that employed protocols that were for the most part severe in
nature in regards to length and/or intensity of the hypoxic stimulus. However, the
elimination of IH in humans with sleep apnea using continuous positive airway pressure (CPAP)
has often been ineffective in mitigating the above mentioned co‐morbidities. The lack of
compliance with CPAP, length of treatment with CPAP (i.e. short durations), and the
possibility that IH or other hallmarks of sleep apnea are not the primary mechanism response
for the listed co‐morbidities, are possible reasons for the absence of improvement in humans.

In contrast to the findings outlined in the previous paragraph, work completed over a similar
time frame indicates that some forms of IH may be beneficial in nature. Many studies using a
variety of protocols and species, including humans, established that exposure to mild IH
initiates sustained increases in the activity of motoneurons, nerves and muscles that
contribute to the enhancement of ventilation and the maintenance of upper airway patency.
This sustained increase has been termed long‐term facilitation (LTF) and this phenomenon has
been the focus of PI's research program for two decades. Long‐term facilitation is the
principle form of respiratory plasticity that we documented in healthy humans, and in humans
with obstructive sleep apnea (OSA) and spinal cord injury (SCI). The initiation of this
phenomenon is mediated by a number of neuromodulators (e.g. serotonin, adenosine,
noradrenaline) that trigger components of at least two cellular pathways, deemed the Q and S
pathways, which mediate the phenomenon. Besides the initiation of LTF, studies in rats and
humans have provided compelling evidence that mild IH might be cardiovascular (e.g.
angiogenesis, reductions in blood pressure, reductions in infarct size), neurocognitive (e.g.
brain neurogenesis, reduced oxidative stress and inflammation) and metabolically (e.g.
decreased cholesterol, decreased low density and very low lipoprotein, increased high density
lipoproteins and reduced hyperglycemia) protective. Many reviews over the past decade,
including reviews from PI's laboratory have addressed the underlying physiological cellular
mechanisms and the translation to whole animals and humans. Briefly, mild IH may lead to
moderate increases in reactive oxygen species. These moderate levels of reactive oxygen
species activate transcription factors (e.g. hypoxia‐inducible factor 1α, nuclear factor
erythroid‐derived 2‐like 2, GATA binding protein 4) that lead to the induction of many
cytoprotective proteins. These proteins serve, for example, to reduce oxidative stress (e.g.
superoxide dismutase, glutathione, thioredoxin), inflammation (e.g. inducible nitric oxide
synthase), apoptosis (e.g. B‐cell lymphoma 2), and promote vasodilation (e.g. heme oxygenase
1) and the formation of blood vessels (e.g. vascular endothelial growth factor). These
modifications that ultimately manifest in improved cardiovascular, autonomic and
neurocognitive outcomes indicate that beneficial responses can be initiated by IH in a dose
dependent fashion without accompanying maladaptive responses. Despite this recognition, the
beneficial responses to IH in humans with sleep apnea have not been fully delineated.

Based on the findings outlined in the previous paragraphs the working hypothesis for the
present proposal is that exposure to mild IH leads to LTF of upper airway muscle activity
that manifests in increased stability of the upper airway, which could ultimately reduce the
CPAP required to treat OSA. As previously reported, a reduction in the therapeutic pressure
necessary for the maintenance of airway patency leads to improved comfort and ultimately
treatment compliance, which is approximately 40 % amongst users. Indeed, the preliminary data
shows that following acute exposure to IH during sleep, and repeated daily exposure to IH
during wakefulness, the therapeutic pressure required for the maintenance of upper airway
patency was significantly reduced during sleep. The reduced therapeutic pressure was also
coupled to a reduction in upper airway resistance and the critical closing pressure. These
modifications ultimately led to increased CPAP compliance. The numerous co‐morbidities listed
in the initial paragraph, which have been linked to hallmarks of sleep apnea (e.g. sleep
fragmentation and severe IH), could be significantly improved by increased compliance to
CPAP. In addition, as outlined above, IH may directly impact on a variety of co‐morbidities
associated with sleep apnea independent of CPAP compliance. Collectively, exposure to IH
could impact on comorbidities linked to sleep apnea both directly and via improved
therapeutic compliance to CPAP.

Thus, our proposal will determine if mild IH can serve as an adjunct therapy coupled to CPAP
to mitigate associated co‐morbidities via its direct effects on a variety of autonomic,
cardiovascular, neurocognitive and metabolic measures and indirectly by improving CPAP
compliance. Autonomic and cardiovascular modifications will be the primary outcome measures
coupled to secondary neurocognitive measures. In addition, metabolic, inflammatory and
angiogenic/vasculogenic biomarkers will be measured to indicate the safety and efficacy of
exposure to IH.

Inclusion Criteria:

- Body mass index < 40 kg/m^2.

- 18 to 60 years old.

- Newly diagnosed sleep apnea (i.e. apnea/hypopnea index < 80 events per hour - average
nocturnal oxygen saturation > 85 %) that has not been treated.

- Diagnosed with prehypertension or Stage 1 hypertension as categorized by the American
Heart Association

- Not pregnant.

- Normal lung function.

- Minimal alcohol consumption (i.e. no more than the equivalent of a glass of wine/day)

- A typical sleep/wake schedule (i.e. participants will not be night shift workers or
have recently travelled across time zones).

Exclusion Criteria:

- Any disease other than high blood pressure and sleep apnea.

- Medications for high blood pressure and sleep promoting supplements including
melatonin

- Current effective CPAP usage (greater than 4 hours per night).

- Night Shift workers or recently traveled across time zones.
We found this trial at
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5050 Anthony Wayne Dr
Detroit, Michigan 48201
(313) 577-2424
Principal Investigator: Jason H Mateika, Ph.D.
Phone: 313-576-4481
Wayne State University Founded in 1868, Wayne State University is a nationally recognized metropolitan research...
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Detroit, Michigan 48201
Principal Investigator: Jason H Mateika, Ph.D.
Phone: 313-576-4481
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Detroit, MI
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