American Journal of Respiratory and Critical Care Medicine

Rationale: Positive airway pressure therapy is frequently used to treat obstructive sleep apnea in children. However, it is not known whether positive airway pressure therapy results in improvements in the neurobehavioral abnormalities associated with childhood sleep apnea.

Objectives: We hypothesized that positive airway pressure therapy would be associated with improvements in attention, sleepiness, behavior, and quality of life, and that changes would be associated with therapy adherence.

Methods: Neurobehavioral assessments were performed at baseline and after 3 months of positive airway pressure therapy in a heterogeneous group of 52 children and adolescents.

Measurements and Main Results: Adherence varied widely (mean use, 170 ± 145 [SD] minutes per night). Positive airway pressure therapy was associated with significant improvements in attention deficits (P < 0.001); sleepiness on the Epworth Sleepiness Scale (P < 0.001); behavior (P < 0.001); and caregiver- (P = 0.005) and child- (P < 0.001) reported quality of life. There was a significant correlation between the decrease in Epworth Sleepiness Scale at 3 months and adherence (r = 0.411; P = 0.006), but not between other behavioral outcomes and adherence. Behavioral factors also improved in the subset of children with developmental delays.

Conclusions: These results indicate that, despite suboptimal adherence use, there was significant improvement in neurobehavioral function in children after 3 months of positive airway pressure therapy, even in developmentally delayed children. The implications for improved family, social, and school function are substantial.

Clinical trial registered with www.clinicaltrials.gov (NCT 00458406).

Scientific Knowledge on the Subject

The childhood obstructive sleep apnea syndrome is common, and some of these children require positive airway pressure therapy. Although neurobehavioral disturbances are important comorbidities of childhood sleep apnea, the efficacy of positive airway pressure therapy in treating these neurobehavioral deficits is unknown.

What This Study Adds to the Field

Our data confirm that neurobehavioral deficits, such as daytime sleepiness, deficits in attention, behavioral problems, and decreased quality of life, are common in children with obstructive sleep apnea. We found that children treated with positive airway pressure therapy exhibited significant improvements in multiple neurobehavioral domains.

The obstructive sleep apnea syndrome (OSAS) affects up to 4% of children (1). In most children, OSAS is associated with adenotonsillar hypertrophy, and improves after adenotonsillectomy (2). However, a significant proportion of children have residual OSAS postoperatively (3). Furthermore, many children with OSAS have other underlying conditions, such as obesity or Down syndrome. In these children, continuous positive airway pressure (CPAP) is usually used as the second line of treatment (2). Although CPAP is now being used commonly in children, only a handful of studies have evaluated its efficacy.

If left untreated, OSAS may lead to substantial comorbidities. In particular, childhood OSAS has been shown to be associated with behavioral disturbances and learning deficits (4). The effect of PAP therapy in treating these neurobehavioral deficits in children is unknown. We therefore prospectively evaluated changes in neurobehavioral parameters, including symptoms of attention-deficit/hyperactivity disorder (ADHD), sleepiness, behavior, and quality of life, at baseline and after 3 months of PAP in children with OSAS. We hypothesized that children treated effectively with PAP, including children with developmental delays, would show improvements in neurobehavioral outcomes.

Some of the results of these studies have been previously reported in the form of an abstract (5).

See the online supplement for additional details.

This study was conducted prospectively as part of a clinical trial comparing two modes of PAP delivery: CPAP versus bilevel pressure release. No difference in adherence or efficacy was found between the modes (6). Children with OSAS aged 2 to 16 years, who were naive to PAP and clinically required PAP, were eligible. The study was approved by the Institutional Review Board of The Children's Hospital of Philadelphia, Philadelphia, Pennsylvania. Written informed consent was obtained from the parent or legal guardian, and assent from children 7 years of age or older when able.

All subjects underwent baseline clinical polysomnography before study entry. Subjects then had a 2-week habituation period at home, followed by a PAP titration study. At the end of 3 months, polysomnography was repeated on PAP, and objective adherence data were downloaded (EncorePro2; Philips Respironics, Murrysville, PA).

Neurobehavioral surveys were administered at baseline and after 3 months of PAP use. Based on known data regarding the domains affected by childhood OSAS, the following were evaluated. (1) Sleepiness, using the Epworth Sleepiness Scale modified for children (79). A score greater than 12 was considered abnormal because it was greater than the 95th percentile for normal children (7). (2) Behavioral problems, using the Child Behavior Checklist (CBCL) (10, 11). This is a survey of behavior competencies that yields standardized, age-adjusted scores on internalizing, externalizing, and total behavior difficulties. Scores between 60 and 63 are borderline; scores greater than 63 are abnormal. (3) ADHD, using the Conners Abbreviated Symptom Questionnaire and the Attention Problems subscale of the CBCL. The Conners scale evaluates inattention, distractibility, and overactivity. Scores range from 0 to 30; greater than or equal to 15 is considered clinically relevant (12). (4) Quality of life was measured using two instruments. The Pediatric Quality of Life Inventory (PedsQL) (13) is a well-validated measure of global quality of life. The score ranges from 0 to 100; the cutoff for moderate to severe impairment in quality of life is greater than 73 for children less than 8 years, and greater than or equal to 65 for children greater than or equal to 8 years (14). The OSAS-18 (15) is a composite of OSAS-related symptoms and disease-specific quality of life. Scores range from 18 to 126. Scores less than 60 suggest a small impact, 60 to 80 suggest a moderate impact, and greater than 80 suggest a large impact of OSAS on quality of life.

Surveys were completed by the same caregiver at each time point. In addition, developmentally able youths aged 11 to 18 completed the CBCL Youth Self Report, and those greater than or equal to 5 years completed the PedsQL.

Statistical Analysis

Unless otherwise specified, data are shown as mean ± SD. Differences between subjects at baseline versus 3 months were analyzed using paired Student t tests, Wilcoxon signed rank tests, or McNemar tests of equality of paired proportions. Differences between those who dropped out and those who completed the study were evaluated using unpaired Student t tests, Mann-Whitney rank sum tests, or Fisher exact test. Pearson or Spearman correlations were used to determine the relationship between adherence and behavioral outcomes. Analysis of covariance models were used to evaluate the effects of demographic variables on neurobehavioral outcomes. P less than 0.05 was considered significant.

Study Group

Details of enrollment have been published elsewhere (6). Sixty subjects were initially enrolled; four were excluded because of medical interventions preventing PAP use, institutionalization, or having moved. Four subjects were lost to follow-up. One subject followed-up with neurocognitive testing but declined repeat polysomnography; this subject was included for analyses other than polysomnography. Thus, 52 subjects completed the study. There were no differences in baseline parameters between those lost to follow-up and those who completed the study.

Details of the study group are shown in Table 1. As is typical for childhood OSAS, where CPAP is usually reserved for children who fail surgical therapy, the study group was heterogeneous, with many children having underlying medical conditions, such as obesity or genetic syndromes (2, 1622). Of note, 19% of subjects had developmental delays (Table 1). Overall, subjects had severe OSAS by pediatric standards (Table 2).

TABLE 1. STUDY GROUP CHARACTERISTICS

N52
Age, yr12 ± 4
Males36 (69)
Race
 African American32 (62)
 White18 (35)
 More than one race2 (4)
Hispanic ethnicity3 (6)
BMI z-score2 ± 0.9
Other diagnoses*
 Obesity36 (69)
 Genetic syndrome9 (17)
 Central nervous system abnormality6 (11)
 Craniofacial syndrome3 (5)
 Pulmonary disease3 (5)
 Growth hormone deficiency1 (2)
Neurodevelopmental disability10 (19)
Maternal education
 Did not complete high school2 (4)
 Completed high school, no college14 (27)
 Some college20 (39)
 Completed college9 (17)
 Completed postgraduate degree7 (14)
PAP adherence
 Nights used over 3 mo60 ± 25
 Average use per night, min170 ± 145

Definition of abbreviations: BMI = body mass index; PAP = positive airway pressure.

Data are shown as mean ± SD or N (%).

* Note that some children had multiple diagnoses.

Obesity defined as BMI greater than or equal to 95th percentile for age and sex (38).

Includes six children with Down syndrome, one with Prader-Willi syndrome, one with cerebral palsy, one with autism, and one with a complex chromosomal disorder.

TABLE 2. POLYSOMNOGRAPHIC DATA (N = 51)

BaselineOn PAPP Value
Sleep efficiency, % total sleep time82 ± 1183 ± 180.81
Arousal index, N/hr23 ± 1516 ± 180.019
Stage N1, % TST8.8 ± 5.96.1 ± 6.7<0.001
Stage N2, % TST49.1 ± 9.946.7 ± 11.20.16
Stage N3, % TST22.3 ± 8.824.6 ± 13.50.18
Rapid eye movement sleep, % TST19.7 ± 6.922.5 ± 7.50.036
Apnea hypopnea index, N/hr18.1 ± 14.72 ± 2.3<0.001
SpO2 nadir, %80 + 1390 ± 4<0.001
Time with SpO2 <90%, % TST4.9 ± 9.10.1 ± 0.50.001
Peak end-tidal CO2, mm Hg57 ± 555 ± 50.027
Time with end-tidal Pco2 >50 mm Hg, % TST16.7 ± 22.412 ± 19.60.42

Definition of abbreviations: PAP = positive airway pressure; SpO2 = oxygen saturation as measured by pulse oximetry; TST = total sleep time.

Data are shown as mean ± SD. Significant P values shown in bold.

Efficacy and Adherence

All subjects had adequate control of their OSAS by PAP on the titration night, with highly significant improvements in respiratory and sleep parameters compared with baseline (Table 2). There was a large variability in adherence, although most subjects attempted to use PAP on most nights (Table 1).

Neurobehavioral Changes

A large number of subjects had neurobehavioral scores in the clinically abnormal range (Table 3). After 3 months of PAP use, there were highly significant improvements in almost all domains (Figures 13). There were significant improvements in symptoms of ADHD (P < 0.001 for the Conner scale and P = 0.005 for the Attention Problems subscale of the CBCL) and daytime sleepiness on the Epworth Sleepiness Scale (P < 0.001). By parental report, internalizing behavior symptoms and total behavior, as measured by the CBCL, improved (both P < 0.001), although externalizing behavior symptoms did not improve (P = 0.181). Twenty-three subjects who were old enough and developmentally able completed the CBCL youth self-report; all three domains improved significantly (P = 0.023 for internalizing symptoms, P < 0.001 for externalizing symptoms, and P = 0.001 for total symptoms). There was an improvement in OSAS-specific (P < 0.001) and general health-related quality of life, as reported by caregivers (P = 0.005) and the children themselves (P < 0.001).

TABLE 3. FREQUENCY OF CHILDREN FALLING IN THE CLINICALLY ABNORMAL RANGE ON NEUROBEHAVIORAL MEASURES AT BASELINE AND AFTER PAP THERAPY

MeasureBaselineOn PAPP Value
Conners Abbreviated Symptom Questionnaire*10 (19.2)6 (11.5)0.289
Modified Epworth Sleepiness Scale14 (26.9)5 (9.6)0.004
Child Behavior Checklist
 Attention problems13 (25)8 (15.4)0.18
 Internalizing13 (25)9 (17.3)0.34
 Externalizing8 (15.4)6 (11.5)0.73
 Total17 (32.7)12 (23.1)0.063
OSAS-18
 Moderate impairment28 (53.8)5 (9.6)<0.001
 Large impairment9 (17.3)2 (3.8)0.039
PedsQL
 Impairment (caregiver report)27 (51.9)16 (30.8)0.013
 Impairment (child report)26 (61.9)13 (31)0.002

Definition of abbreviations: OSAS = obstructive sleep apnea syndrome; PAP = positive airway pressure.

Data are shown as N (%). P values are based on McNemar tests of equality of paired proportions. Significant P values shown in bold.

* N = 51.

N = 42.

The percentage of children with scores in the clinically abnormal range decreased on PAP for all domains, with significant reductions seen in the percentage of children with pathologic sleepiness on the Epworth Sleepiness Scale, and with low quality of life (Table 3).

The effect of age, sex, race, body mass index z-score, maternal education, and baseline scores on neurobehavioral outcomes was assessed. Baseline scores had a significant effect for all outcomes (P = 0.002 for OSA-18; P < 0.0005 for all other outcomes). Other than baseline scores, the only other significant effect was for sex on the change in score of the internalizing symptoms of the CBCL, with girls showing a greater improvement than boys (−6.9 ± 6.9 vs. −2.3 ± 7.9, respectively; P = 0.049).

To assess the relationship between the degree of adherence and behavioral outcomes, the correlation between adherence parameters and behavioral outcomes was measured. There was a significant correlation between the change in the Epworth Sleepiness Scale score at 3 months and PAP adherence (mean minutes used per night, r = −0.411, P = 0.006; nights used, r = −0.348, P = 0.028) (Figure 4), but no significant correlation between other behavioral outcomes and PAP use.

Subjects with developmental delays.

Ten subjects had significant developmental delays. Exploratory analyses were performed for this small subset of children. There were similar findings to the total study group, with significant improvements in the Epworth Sleepiness Scale (P = 0.003), internalizing (P = 0.024), and total behavior scores (P = 0.049), and OSAS-specific (P = 0.001) and general (P = 0.037) quality of life.

Subjects younger than 7 years of age.

Because PAP is not approved by the Food and Drug Administration for children less than 7 years of age or weighing less than 40 lb (18 kg), this subgroup was evaluated separately in exploratory analyses. In this small subset (n = 7; age 4.5 ± 1.7 yr; range, 2–6 yr), significant improvements were found in sleepiness on the Epworth Sleepiness Scale (P = 0.012) and OSAS-specific quality of life (P = 0.021).

PAP use is known to be highly effective at treating OSAS as demonstrated on polysomnograpy (18). However, the clinical benefits of using PAP in children have not been well-studied. It is very difficult to get young children to wear the PAP apparatus (18, 2123). Furthermore, many children requiring PAP therapy have underlying chronic illnesses or developmental delays (2, 1622), further complicating efforts to improve adherence. It is therefore imperative to show that PAP use actually improves clinical outcomes in addition to improving polysomnographic abnormalities, before widespread pediatric PAP programs can be advocated. This study showed that PAP use was associated with significant changes in neurobehavioral parameters after only 3 months of use, even in a heterogeneous group of children with OSAS, including very young children and children with developmental delays. In addition to statistically significant improvements in neurobehavioral parameters, there was a reduction in the number of children falling into the clinically abnormal range (Table 3).

In adults, OSAS is associated with a wide range of neurocognitive deficits. These include deficits in daytime sleepiness, mood, cognitive processing, sustained attention, executive functioning, short-term working memory, and quality of life, all of which lead to diminished ability to execute various activities of daily living, such as occupational performance, driving safety, and psychosocial functioning (24, 25). However, in adults PAP use has not been clearly shown to improve many of these deficits (25, 26). A possible explanation for the improvement in function seen in children in the current study compared with the studies of adults may be that the children had a shorter duration of OSAS and therefore increased reversibility. Another explanation may be the increased plasticity of the child's central nervous system. The improvements may have been caused by improvements in gas exchange during sleep and improvements in sleep fragmentation.

Although neurobehavioral consequences of OSAS have been investigated extensively in adults, the consequences in children have not been fully evaluated. There is emerging evidence that children with OSAS show deficits in neurocognitive performance, behavioral impairments, and reduced school performance (4, 2732), similar to those noted in the current study. Several studies have shown that these neurocognitive and behavioral abnormalities are at least partially reversible with surgical treatment in otherwise healthy children (27, 30, 3335), although these studies were limited by small sample sizes or lack of full polysomnography. Only a handful of studies have examined the impact of PAP therapy on daytime functioning in children with OSAS. A study of 13 obese adolescents with OSAS found improvements in school performance, vigilance, and school-related quality of life in those who were adherent to PAP (36). Another study only evaluated subjective measures, and found improvements in sleepiness but no change in subjective assessments of attention or behavior (18).

In this study, changes in behavioral function were seen after only 3 months of PAP use. The time required for maximal improvements in behavioral function is unknown but may well be longer than 3 months, and further studies with long-term follow-up are needed.

The use of PAP therapy with children can be challenging despite close follow-up and support. In the current study, there was considerable variability in PAP adherence among subjects, with low overall adherence, consistent with findings from previous studies (18, 21, 22, 36). Despite this, improvements were found in all neurobehavioral domains. Conceivably, better adherence would result in even further improvements. Surprisingly, however, a significant correlation between improvements and adherence was found only in regards to daytime sleepiness, as measured on the Epworth Sleepiness Scale. Similarly, in adults, sleepiness improves in response to increased CPAP use (37). One reason for the lack of correlation between PAP use and other neurobehavioral outcomes in the current study may be the difference in physiologic sleep requirements over the age spectrum studied, and the differing degree of baseline neurobehavioral function in the subjects. Thus, the effects of wearing CPAP for 4 hours a night may be less beneficial in a 2 year old sleeping for 12 hours a night than in a 16 year old sleeping 8 hours a night.

In adults, 4 hours of PAP use per night is traditionally considered to be adequate adherence. The current study suggests that, in children, the longer the PAP mask is worn, the better the outcomes (at least in regards to daytime sleepiness). However, some benefit can be obtained from even small amounts of PAP use. Thus, any degree of PAP use should be encouraged.

In the current study, even children with significant developmental delays showed an improvement in some parameters with PAP. Therefore, PAP is recommended for this patient population, to optimize each child's potential. Note that the study was underpowered for the developmentally delayed subjects subset and the subset of children younger than 7 years of age, and may thus have missed other changes in behavioral parameters. Further studies of these high-risk groups are warranted.

A limitation of this study is that a placebo group was not included, and reports from individuals other than the subjects (for some measures) and caregivers, such as teachers, were not obtained. Subjects and their caregivers were not masked as to PAP treatment, and this may have impacted the responses to the surveys used as outcome measures.

The inclusion of children with a variety of underlying medical conditions and across the age spectrum is a limitation and strength of this study. This is the first comprehensive study of the effects of PAP use in children, and thus the study was designed to include the typical pediatric patient populations requiring PAP therapy. The study results are directly applicable to clinical pediatric sleep medicine practice. Further studies evaluating more homogeneous study groups are warranted to more closely determine the relationship between PAP use and neurobehavioral outcomes.

In conclusion, the treatment of childhood OSAS with PAP therapy was associated with significant improvements in daytime sleepiness, symptoms of ADHD, internalizing behaviors, and quality of life in children with OSAS, including young children and children with developmental delays. These improvements occurred despite a mean use of only 3 hours per night, suggesting that clinicians should encourage any PAP use, and not be discouraged when adherence is suboptimal. These findings have important implications in managing children with OSAS, because reinforcing PAP use is beneficial in many domains of daily life.

The authors thank all the children and families who participated in this study, and the sleep technologists for their dedication and professionalism.

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Correspondence and requests for reprints should be addressed to Carole L. Marcus, M.B.B.Ch., Children's Hospital of Philadelphia, Main Building, 9NW50, 34th Street and Civic Center Boulevard, Philadelphia, PA 19104. E-mail:

Supported by Philips Respironics. All data collection, statistical analyses, and manuscript writing were performed by the investigators independent of Philips Respironics. C.L.M. also received support from NIH HL58585, and L.J.M. from K23 MH077662.

Author Contributions: C.L.M. was the principal investigator and responsible for all aspects of study design, data collection, data analysis, and manuscript preparation. J.R. and L.J.M. helped with the selection and interpretation of the social and psychometric survey instruments and were involved in study design, data analysis, and manuscript preparation. S.K. assisted with data analyses and manuscript preparation. S.E.B. was the unblinded physician safety monitor. M.A.C. and L.R.K. were study coordinators and participated in subject recruitment, data collection, and data entry. J.T. managed the database and adherence data collection and analysis. N.D. was study nurse and provided subject evaluation and support, fitted equipment, evaluated and managed side effects in conjunction with study physicians, and provided behavioral counseling for continuous positive airway pressure use. P.R.G. was responsible for statistical analyses and was involved in study design and manuscript preparation.

This article has an online supplement, which is accessible from this issue's table of contents at www.atsjournals.org

Originally Published in Press as DOI: 10.1164/rccm.201112-2167OC on February 9, 2012

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