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Sleep-Disordered Breathing and Transcranial Dopplers in Sickle Cell Disease

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ARCHIVES OF OTOLARYNGOLOGY-HEAD & NECK SURGERY
卷 137, 期 12, 页码 1263-1268

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AMER MEDICAL ASSOC
DOI: 10.1001/archoto.2011.190

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Objectives: To determine the prevalence of sleep-disordered breathing in children with sickle cell disease and whether there is an association of sleep-disordered breathing with high-risk transcranial Doppler ultrasonography (TCD) velocities. Study Design: Cross-sectional. Setting: Tertiary care academic medical center. Patients: Sixty-four children (aged 2-14 years) selected for eligible genotype (type SS or S beta(0)-thalassemia) and no history of stroke. Interventions: Parents completed the Pediatric Sleep Questionnaire. Overnight polysomnography was performed for children with snoring. The TCD was performed or existing results were obtained for all children; for children who underwent transfusion therapy, readings prior to the transfusion were analyzed. Children with abnormal or conditional TCD (flow velocity >= 170 cm/s in any vessel) were considered high risk. Main Outcome Measures: Prevalence of sleep-disordered breathing and TCD velocity and frequency of high-risk TCD in patients with and without sleep-disordered breathing. Results: The prevalence of snoring was 37.5% (95% CI, 26.7%-49.8%), the prevalence of positive polysomnography findings was 23.7% (14.6%-36.1%), and the prevalence of positive Pediatric Sleep Questionnaire scores was 21.9% (13.4%-33.6%). There was no significant difference in TCD velocity or number of patients with high-risk TCD between nonsnorers and children with snoring but negative polysomnography findings and children with snoring and positive polysomnography findings (P=.91 and P=.66, respectively) or between nonsnorers and snorers with a negative Pediatric Sleep Questionnaire score and snorers with a positive Pediatric Sleep Questionnaire score (P=.76 and P=.33, respectively). Conclusion: There is a high prevalence of snoring and sleep-disordered breathing among children with sickle cell disease, but our results do not support an association with cerebrovascular risk.

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