Novel Associations of Multiple Genetic Loci With Plasma Levels of Factor VII, Factor VIII, and von Willebrand Factor

医学 血管性血友病因子 因子(编程语言) 内科学 遗传学 血小板 生物 计算机科学 程序设计语言
作者
Nicholas L. Smith,Ming‐Huei Chen,Abbas Dehghan,David P. Strachan,Saonli Basu,Nicole Soranzo,Caroline Hayward,Igor Rudan,Maria Sabater‐Lleal,Joshua C. Bis,Moniek P.M. de Maat,Ann Rumley,Xiaoxiao Kong,Qiong Yang,Frances M. K. Williams,Véronique Vitart,Harry Campbell,Anders Mälarstig,Kerri L. Wiggins,Cornelia M. van Duijn,Wendy L. McArdle,James S. Pankow,Andrew D. Johnson,Angela Silveira,Barbara McKnight,André G. Uitterlinden,Nena Aleksic,James B. Meigs,Annette Peters,Wolfgang Köenig,Mary Cushman,Sekar Kathiresan,Jerome I. Rotter,Edwin G. Bovill,Albert Hofman,Eric Boerwinkle,Geoffrey H. Tofler,John F. Peden,Bruce M. Psaty,Frank W.G. Leebeek,Aaron R. Folsom,Martin G. Larson,Timothy D. Spector,Alan F. Wright,James F. Wilson,Anders Hamsten,Thomas Lumley,Jacqueline C.M. Witteman,Weihong Tang,Christopher J. O’Donnell
出处
期刊:Circulation [Ovid Technologies (Wolters Kluwer)]
卷期号:121 (12): 1382-1392 被引量:345
标识
DOI:10.1161/circulationaha.109.869156
摘要

Plasma levels of coagulation factors VII (FVII), VIII (FVIII), and von Willebrand factor (vWF) influence risk of hemorrhage and thrombosis. We conducted genome-wide association studies to identify new loci associated with plasma levels.The setting of the study included 5 community-based studies for discovery comprising 23 608 European-ancestry participants: Atherosclerosis Risk In Communities Study, Cardiovascular Health Study, British 1958 Birth Cohort, Framingham Heart Study, and Rotterdam Study. All subjects had genome-wide single-nucleotide polymorphism (SNP) scans and at least 1 phenotype measured: FVII activity/antigen, FVIII activity, and vWF antigen. Each study used its genotype data to impute to HapMap SNPs and independently conducted association analyses of hemostasis measures using an additive genetic model. Study findings were combined by meta-analysis. Replication was conducted in 7604 participants not in the discovery cohort. For FVII, 305 SNPs exceeded the genome-wide significance threshold of 5.0x10(-8) and comprised 5 loci on 5 chromosomes: 2p23 (smallest P value 6.2x10(-24)), 4q25 (3.6x10(-12)), 11q12 (2.0x10(-10)), 13q34 (9.0x10(-259)), and 20q11.2 (5.7x10(-37)). Loci were within or near genes, including 4 new candidate genes and F7 (13q34). For vWF, 400 SNPs exceeded the threshold and marked 8 loci on 6 chromosomes: 6q24 (1.2x10(-22)), 8p21 (1.3x10(-16)), 9q34 (<5.0x10(-324)), 12p13 (1.7x10(-32)), 12q23 (7.3x10(-10)), 12q24.3 (3.8x10(-11)), 14q32 (2.3x10(-10)), and 19p13.2 (1.3x10(-9)). All loci were within genes, including 6 new candidate genes, as well as ABO (9q34) and VWF (12p13). For FVIII, 5 loci were identified and overlapped vWF findings. Nine of the 10 new findings were replicated.New genetic associations were discovered outside previously known biological pathways and may point to novel prevention and treatment targets of hemostasis disorders.

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