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Pediatric Asthma

Pediatric sleep questionnaire predicts more severe sleep apnea in children with uncontrolled asthma

, DO, , MS, , MSN, , MD, , MD, , MD, , MD, , BA, , BA, , BS, , MD & , MD show all
Pages 1589-1596 | Received 10 Jun 2020, Accepted 30 Aug 2020, Published online: 14 Sep 2020
 

Abstract

Objective

While up to 35% of children with asthma have evidence of sleep disordered breathing (SDB), it is unclear if nocturnal symptoms stem from asthma itself or SDB. The Pediatric Sleep Questionnaire (PSQ) is a validated tool for identifying SDB in childhood asthma. We hypothesize children with asthma and abnormal PSQ demonstrate decreased asthma control and are at higher risk of obstructive sleep apnea (OSA).

Methods

We performed a retrospective, chart review of children and young adults referred to our tertiary children’s hospital severe asthma clinic. Data collection included age, gender, BMI percentile, spirometry, PSQ, asthma control questionnaires, asthma severity, control, and impairment. These data were evaluated in the context of polysomnography, when available.

Results

205 inner-city children were included; 37.2% female, median age 6.4 y, and mean BMI of 71.3%ile. Rhinitis (p = 0.028), eczema (p = 0.002), and reflux (p = 0.046) were associated with abnormal PSQ; however, overweight/obese status, spirometry, asthma severity, and serologic markers were not. After correcting for comorbidities, abnormal PSQ score was associated with poor asthma control based on validated measures (p < 0.001). In patients with polysomnography, we confirmed abnormal PSQ was associated with increased OSA severity (apnea-hypopnea index 9.1/hr vs. 3.6/hr; p = 0.027).

Conclusions

In pediatric asthma, positive PSQ was associated with significantly decreased asthma control. Additionally, children with normal PSQ demonstrated mild OSA, while children with abnormal PSQ had increased severity of OSA. This demonstrates that PSQ can be used to screen children for more severe sleep apnea.

Declaration of interest

The authors report no conflict of interest

Additional information

Funding

This work was supported by NIH/NIBIB (grant no. 1U01EB021986 (DKP)).

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