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α2-Adrenergic blockade rescues hypoglossal motor defense against obstructive sleep apnea
Gang Song, Chi-Sang Poon
Gang Song, Chi-Sang Poon
Published February 23, 2017
Citation Information: JCI Insight. 2017;2(4):e91456. https://doi.org/10.1172/jci.insight.91456.
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Research Article Neuroscience Pulmonology

α2-Adrenergic blockade rescues hypoglossal motor defense against obstructive sleep apnea

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Abstract

Decreased noradrenergic excitation of hypoglossal motoneurons during sleep causing hypotonia of pharyngeal dilator muscles is a major contributor to the pathogenesis of obstructive sleep apnea (OSA), a widespread disease for which treatment options are limited. Previous OSA drug candidates targeting various excitatory/inhibitory receptors on hypoglossal motoneurons have proved unviable in reactivating these neurons, particularly during rapid-eye-movement (REM) sleep. To identify a viable drug target, we show that the repurposed α2-adrenergic antagonist yohimbine potently reversed the depressant effect of REM sleep on baseline hypoglossal motoneuron activity (a first-line motor defense against OSA) in rats. Remarkably, yohimbine also restored the obstructive apnea–induced long-term facilitation of hypoglossal motoneuron activity (hLTF), a much-neglected form of noradrenergic-dependent neuroplasticity that could provide a second-line motor defense against OSA but was also depressed during REM sleep. Corroborating immunohistologic, optogenetic, and pharmacologic evidence confirmed that yohimbine’s beneficial effects on baseline hypoglossal motoneuron activity and hLTF were mediated mainly through activation of pontine A7 and A5 noradrenergic neurons. Our results suggest a 2-tier (impaired first- and second-line motor defense) mechanism of noradrenergic-dependent pathogenesis of OSA and a promising pharmacotherapy for rescuing both these intrinsic defenses against OSA through disinhibition of A7 and A5 neurons by α2-adrenergic blockade.

Authors

Gang Song, Chi-Sang Poon

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Figure 4

Pontine A7 and A5 noradrenergic neuronal groups were activated by episodic obstructive apnea.

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Pontine A7 and A5 noradrenergic neuronal groups were activated by episod...
(A) Photomicrographs showing A7 and A5 noradrenergic neurons identified by dopamine β-hydroxylase (DBH) immunofluorescent labeling that were immunopositive to c-Fos in a rat exposed to episodic obstructive apnea, compared with one that was not exposed (control). “×” indicates artifacts; arrows indicate doubly labeled neurons. (B) Percentage of c-Fos immunopositive neurons among A7, A5, or A6 noradrenergic neurons in the experimental group (n = 6) and control group (n = 3). LC, locus coeruleus; SubC, subcoeruleus. *P < 0.05 between values as indicated, 2-tailed Student’s t test.

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