Whole-genome association analyses of sleep-disordered breathing phenotypes in the NHLBI TOPMed program

遗传建筑学 全基因组关联研究 遗传学 遗传关联 睡眠呼吸暂停 表型 生物 阻塞性睡眠呼吸暂停 医学 生物信息学 单核苷酸多态性 基因型 基因 内科学
作者
Brian E. Cade,Jiwon Lee,Tamar Sofer,Heming Wang,Man Zhang,Han Chen,Sina A. Gharib,Daniel J. Gottlieb,Xiuqing Guo,Jacqueline M. Lane,Jingjing Liang,Xihong Lin,Hao Mei,Sanjay R. Patel,Shaun Purcell,Richa Saxena,Neomi Shah,Daniel S. Evans,Craig L. Hanis,David R. Hillman,Sutapa Mukherjee,Lyle J. Palmer,Katie L. Stone,Gregory J. Tranah,Namiko Abe,Gonçalo R. Abecasis,Christine M. Albert,Laura Almasy,Álvaro Alonso,Seth A. Ament,Peter H. Anderson,Pramod Anugu,Deborah Applebaum‐Bowden,Dan E. Arking,Donna K. Arnett,Allison E. Ashley‐Koch,Stella Aslibekyan,Tim Assimes,Paul L. Auer,Dimitrios Avramopoulos,J. A. Barnard,Kathleen C. Barnes,R. Graham Barr,Emily Barron‐Casella,Terri Beaty,Diane M. Becker,Lewis C. Becker,Rebecca Beer,Ferdouse Begum,Amber L. Beitelshees,Emelia J. Benjamin,Marcos Bezerra,Larry Bielak,Joshua Bis,Thomas W. Blackwell,John Blangero,Eric Boerwinkle,Ingrid Borecki,Donald W. Bowden,Russell P. Bowler,Jennifer A. Brody,Ulrich Broeckel,Jai Broome,Karen Bunting,Esteban G. Burchard,Brian E. Cade,Jonathan Cardwell,Cara L. Carty,Richard Casaburi,James F. Casella,Mark Chaffin,Christy Chang,Daniel I. Chasman,Sameer Chavan,Bo-Juen Chen,Wei‐Min Chen,Yii‐Der Ida Chen,Michael H. Cho,Seung Hoan Choi,Lee‐Ming Chuang,Mina K. Chung,Elaine Cornell,Adolfo Correa,Carolyn Crandall,James D. Crapo,L. Adrienne Cupples,Joanne E. Curran,Jeffrey R. Curtis,Brian Custer,Coleen Damcott,Dawood Darbar,Sayantan Das,Sean P. David,Colleen Davis,Michelle Daya,Mariza de Andrade,Michael R. DeBaun,Ranjan Deka,Dawn L. DeMeo,Scott E. Devine
出处
期刊:Genome Medicine [Springer Nature]
卷期号:13 (1) 被引量:20
标识
DOI:10.1186/s13073-021-00917-8
摘要

Sleep-disordered breathing is a common disorder associated with significant morbidity. The genetic architecture of sleep-disordered breathing remains poorly understood. Through the NHLBI Trans-Omics for Precision Medicine (TOPMed) program, we performed the first whole-genome sequence analysis of sleep-disordered breathing.The study sample was comprised of 7988 individuals of diverse ancestry. Common-variant and pathway analyses included an additional 13,257 individuals. We examined five complementary traits describing different aspects of sleep-disordered breathing: the apnea-hypopnea index, average oxyhemoglobin desaturation per event, average and minimum oxyhemoglobin saturation across the sleep episode, and the percentage of sleep with oxyhemoglobin saturation < 90%. We adjusted for age, sex, BMI, study, and family structure using MMSKAT and EMMAX mixed linear model approaches. Additional bioinformatics analyses were performed with MetaXcan, GIGSEA, and ReMap.We identified a multi-ethnic set-based rare-variant association (p = 3.48 × 10-8) on chromosome X with ARMCX3. Additional rare-variant associations include ARMCX3-AS1, MRPS33, and C16orf90. Novel common-variant loci were identified in the NRG1 and SLC45A2 regions, and previously associated loci in the IL18RAP and ATP2B4 regions were associated with novel phenotypes. Transcription factor binding site enrichment identified associations with genes implicated with respiratory and craniofacial traits. Additional analyses identified significantly associated pathways.We have identified the first gene-based rare-variant associations with objectively measured sleep-disordered breathing traits. Our results increase the understanding of the genetic architecture of sleep-disordered breathing and highlight associations in genes that modulate lung development, inflammation, respiratory rhythmogenesis, and HIF1A-mediated hypoxic response.
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