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Clinical Trial
. 2015 Apr;8(2):398-409.
doi: 10.1161/CIRCGENETICS.114.000858. Epub 2015 Feb 7.

Multiethnic genome-wide association study of cerebral white matter hyperintensities on MRI

Benjamin F J VerhaarenStéphanie DebetteJoshua C BisJennifer A SmithM Kamran IkramHieab H AdamsAshley H BeechamKumar B RajanLorna M LopezSandra BarralMark A van BuchemJeroen van der GrondAlbert V SmithKatrin HegenscheidNeelum T AggarwalMariza de AndradeElizabeth J AtkinsonMarian BeekmanAlexa S BeiserSusan H BlantonEric BoerwinkleAdam M BrickmanR Nick BryanGanesh ChauhanChristopher P L H ChenVincent ChourakiAnton J M de CraenFabrice CrivelloIan J DearyJoris DeelenPhilip L De JagerCarole DufouilMitchell S V ElkindDenis A EvansPaul FreudenbergerRebecca F GottesmanVilmundur GuðnasonMohamad HabesSusan R HeckbertGerardo HeissSaima HilalEdith HoferAlbert HofmanCarla A Ibrahim-VerbaasDavid S KnopmanCora E LewisJiemin LiaoDavid C M LiewaldMichelle LucianoAad van der LugtOliver O MartinezRichard MayeuxBernard MazoyerMike NallsMatthias NauckWiro J NiessenBen A OostraBruce M PsatyKenneth M RiceJerome I RotterBettina von SarnowskiHelena SchmidtPamela J SchreinerMaaike SchuurStephen S SidneySigurdur SigurdssonP Eline SlagboomDavid J M StottJohn C van SwietenAlexander TeumerAnna Maria TöglhoferMatthew TraylorStella TrompetStephen T TurnerChristophe TzourioHae-Won UhAndré G UitterlindenMeike W VernooijJing J WangTien Y WongJoanna M WardlawB Gwen WindhamKatharina WittfeldChristiane WolfClinton B WrightQiong YangWei ZhaoAlex ZijdenbosJ Wouter JukemaRalph L SaccoSharon L R KardiaPhilippe AmouyelThomas H MosleyW T Longstreth JrCharles C DeCarliCornelia M van DuijnReinhold SchmidtLenore J LaunerHans J GrabeSudha S SeshadriM Arfan IkramMyriam Fornage
Clinical Trial

Multiethnic genome-wide association study of cerebral white matter hyperintensities on MRI

V体育安卓版 - Benjamin F J Verhaaren et al. Circ Cardiovasc Genet. 2015 Apr.

Abstract

Background: The burden of cerebral white matter hyperintensities (WMH) is associated with an increased risk of stroke, dementia, and death. WMH are highly heritable, but their genetic underpinnings are incompletely characterized. To identify novel genetic variants influencing WMH burden, we conducted a meta-analysis of multiethnic genome-wide association studies VSports手机版. .

Methods and results: We included 21 079 middle-aged to elderly individuals from 29 population-based cohorts, who were free of dementia and stroke and were of European (n=17 936), African (n=1943), Hispanic (n=795), and Asian (n=405) descent. WMH burden was quantified on MRI either by a validated automated segmentation method or a validated visual grading scale. Genotype data in each study were imputed to the 1000 Genomes reference. Within each ethnic group, we investigated the relationship between each single-nucleotide polymorphism and WMH burden using a linear regression model adjusted for age, sex, intracranial volume, and principal components of ancestry. A meta-analysis was conducted for each ethnicity separately and for the combined sample. In the European descent samples, we confirmed a previously known locus on chr17q25 (P=2. 7×10(-19)) and identified novel loci on chr10q24 (P=1. 6×10(-9)) and chr2p21 (P=4. 4×10(-8)). In the multiethnic meta-analysis, we identified 2 additional loci, on chr1q22 (P=2. 0×10(-8)) and chr2p16 (P=1. 5×10(-8)). The novel loci contained genes that have been implicated in Alzheimer disease (chr2p21 and chr10q24), intracerebral hemorrhage (chr1q22), neuroinflammatory diseases (chr2p21), and glioma (chr10q24 and chr2p16) V体育安卓版. .

Conclusions: We identified 4 novel genetic loci that implicate inflammatory and glial proliferative pathways in the development of WMH in addition to previously proposed ischemic mechanisms. V体育ios版.

Keywords: cerebral small vessel diseases; cerebrovascular disorders; genome-wide association study; hypertension; leukoencephalopathies; polymorphisms, single nucleotide VSports最新版本. .

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VSports手机版 - Conflict of interest statement

Conflict of Interest Disclosures: None

Figures (VSports)

Figure 1
Figure 1
Regional plots of the genome-wide significant loci in individuals of European descent. Loci on chr17q25.1, chr10q24.33, chr2p16.1, chr1q22 and chr2p21 are shown. Each circle indicates a SNP with a color scale corresponding to the r2value for that SNP and the top SNP from 1000 Genomes. Purple diamonds indicate the SNPs with the strongest association in the overall meta-analysis. Estimated recombination from 1000 Genomes are indicated blue lines. The bottom panels show the relative position of genes within each locus.

References

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