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[Preprint]. 2024 Sep 4:2024.09.02.24312466.
doi: 10.1101/2024.09.02.24312466.

A Large-Scale Genome-Wide Gene-Sleep Interaction Study in 732,564 Participants Identifies Lipid Loci Explaining Sleep-Associated Lipid Disturbances

Raymond NoordamWenyi WangPavithra NagarajanHeming WangMichael R BrownAmy R BentleyQin HuiAldi T KrajaJohn L MorrisonJeffrey R O'ConnelSongmi LeeKaren SchwanderTraci M BartzLisa de las FuentesMary F FeitosaXiuqing GuoXu HanfeiSarah E HarrisZhijie HuangMart KalsChristophe LefevreMassimo ManginoYuri MilaneschiPeter van der MostNatasha L PachecoNicholette D PalmerVarun RaoRainer RauramaaQuan SunYasuharu TabaraDina VojinovicYujie WangStefan WeissQian YangWei ZhaoWanying ZhuMd Abu Yusuf AnsariHugues AschardPramod AnuguThemistocles L AssimesJohn AttiaLaura D BakerChristie BallantyneLydia BazzanoEric BoerwinkleBrain CadeHung-Hsin ChenWei ChenYii-Der Ida ChenZekai ChenKelly ChoIleana De Anda-DuranLatchezar DimitrovAnh DoTodd EdwardsTariq FaquihAroon HingoraniSusan P Fisher-HochJ Michael GazianoSina A GharibAyush GiriMohsen GhanbariHans Jörgen GrabeMariaelisa GraffC Charles GuJiang HeSami HeikkinenJames HixsonYuk-Lam HoMichelle M HoodSerena C HoughtonCarrie A Karvonen-GutierrezTakahisa KawaguchiTuomas O KilpeläinenPirjo KomulainenHenry J LinGregorio V LinchangcoAnnemarie I LuikJintao MaJames B MeigsJoseph B McCormickCristina MenniIlja M NolteJill M NorrisLauren E PettyHannah G PolikowskyLaura M RaffieldStephen S RichRenata L RihaThomas C RussEdward A Ruiz-NarvaezColleen M SitlaniJennifer A SmithHarold SniederTamar SoferBotong ShenJingxian TangKent D TaylorMaris Teder-LavingRima TriatinMichael Y TsaiHenry VölzkeKenneth E WestermanRui XiaJie YaoKristin L YoungRuiyuan ZhangAlan B ZondermanXiaofeng ZhuJennifer E BelowSimon R CoxMichelle EvansMyriam FornageErvin R FoxNora FranceschiniSioban D HarlowElizabeth HollidayM Arfan IkramTanika KellyTimo A LakkaDeborah A LawlorChangwei LiChing-Ti LiuReedik MägiAlisa K ManningFumihiko MatsudaAlanna C MorrisonMatthias NauckKari E NorthBrenda Wjh PenninxMichael A ProvinceBruce M PsatyJerome I RotterTim D SpectorLynne E WagenknechtKo Willems van DijkLifelines Cohort StudyMillion Veteran ProgramCashell E JaquishPeter Wf WilsonPatricia A PeyserPatricia B MunroePaul S de VriesW James GaudermanYan V SunHan ChenClint L MillerThomas W WinklerDabeeru C RaoSusan RedlineDiana van Heemst

A Large-Scale Genome-Wide Gene-Sleep Interaction Study in 732,564 Participants Identifies Lipid Loci Explaining Sleep-Associated Lipid Disturbances

Raymond Noordam et al. medRxiv. .

Abstract

We performed large-scale genome-wide gene-sleep interaction analyses of lipid levels to identify novel genetic variants underpinning the biomolecular pathways of sleep-associated lipid disturbances and to suggest possible druggable targets. We collected data from 55 cohorts with a combined sample size of 732,564 participants (87% European ancestry) with data on lipid traits (high-density lipoprotein [HDL-c] and low-density lipoprotein [LDL-c] cholesterol and triglycerides [TG]). Short (STST) and long (LTST) total sleep time were defined by the extreme 20% of the age- and sex-standardized values within each cohort. Based on cohort-level summary statistics data, we performed meta-analyses for the one-degree of freedom tests of interaction and two-degree of freedom joint tests of the main and interaction effect. In the cross-population meta-analyses, the one-degree of freedom variant-sleep interaction test identified 10 loci (P int <5.0e-9) not previously observed for lipids. Of interest, the ASPH locus (TG, LTST) is a target for aspartic and succinic acid metabolism previously shown to improve sleep and cardiovascular risk. The two-degree of freedom analyses identified an additional 7 loci that showed evidence for variant-sleep interaction (P joint <5.0e-9 in combination with P int <6.6e-6). Of these, the SLC8A1 locus (TG, STST) has been considered a potential treatment target for reduction of ischemic damage after acute myocardial infarction. Collectively, the 17 (9 with STST; 8 with LTST) loci identified in this large-scale initiative provides evidence into the biomolecular mechanisms underpinning sleep-duration-associated changes in lipid levels. The identified druggable targets may contribute to the development of novel therapies for dyslipidemia in people with sleep disturbances.

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