Genetic investigation of fibromuscular dysplasia identifies risk loci and shared genetics with common cardiovascular diseases.
Adrien GeorgesMin-Lee YangTakiy-Eddine BerrandouMark K BakkerOzan DikilitasSoto Romuald KiandoLijiang MaBenjamin A SatterfieldSebanti SenguptaMengyao YuJean François DeleuzeDelia DupréKristina L HunkerSergiy KyryachenkoLu LiuInes Sayoud-SadegLaurence AmarChad M BrummettDawn M ColemanValentina d'EscamardPeter W de LeeuwNatalia Fendrikova-MahlayDaniella Kadian-DodovJun Z LiAurélien LorthioirMarco PappaccogliAleksander PrejbiszWitold SmigielskiJames C StanleyMatthew ZawistowskiXiang ZhouSebastian Zöllnernull nullnull nullnull nullPhillippe AmouyelMarc L De BuyzereStephanie DebettePiotr DobrowolskiWojciech DrygasHeather L GornikJeffrey W OlinJerzy PiwonskiErnst R RietzschelYnte M RuigrokMiikka VikkulaEwa Warchol CelinskaAndrzej JanuszewiczIftikhar J KulloMichel AziziXavier JeunemaitreAlexandre PersuJason C KovacicSanthi K GaneshNabila Bouatia-NajiPublished in: Nature communications (2021)
Fibromuscular dysplasia (FMD) is an arteriopathy associated with hypertension, stroke and myocardial infarction, affecting mostly women. We report results from the first genome-wide association meta-analysis of six studies including 1556 FMD cases and 7100 controls. We find an estimate of SNP-based heritability compatible with FMD having a polygenic basis, and report four robustly associated loci (PHACTR1, LRP1, ATP2B1, and LIMA1). Transcriptome-wide association analysis in arteries identifies one additional locus (SLC24A3). We characterize open chromatin in arterial primary cells and find that FMD associated variants are located in arterial-specific regulatory elements. Target genes are broadly involved in mechanisms related to actin cytoskeleton and intracellular calcium homeostasis, central to vascular contraction. We find significant genetic overlap between FMD and more common cardiovascular diseases and traits including blood pressure, migraine, intracranial aneurysm, and coronary artery disease.
Keyphrases
- genome wide
- blood pressure
- copy number
- dna methylation
- genome wide association
- cardiovascular disease
- coronary artery disease
- induced apoptosis
- heart failure
- atrial fibrillation
- transcription factor
- minimally invasive
- cardiovascular risk factors
- type diabetes
- percutaneous coronary intervention
- metabolic syndrome
- pregnant women
- pregnancy outcomes
- cell migration
- signaling pathway
- insulin resistance
- blood brain barrier
- cervical cancer screening
- bioinformatics analysis