4 research outputs found
Shared genetic susceptibility to ischemic stroke and coronary artery disease : a genome-wide analysis of common variants
Get PDFBackground and Purpose-Ischemic stroke (IS) and coronary artery disease (CAD) share several risk factors and each has a substantial heritability. We conducted a genome-wide analysis to evaluate the extent of shared genetic determination of the two diseases. Methods-Genome-wide association data were obtained from the METASTROKE, Coronary Artery Disease Genomewide Replication and Meta-analysis (CARDIoGRAM), and Coronary Artery Disease (C4D) Genetics consortia. We first analyzed common variants reaching a nominal threshold of significance (P<0.01) for CAD for their association with IS and vice versa. We then examined specific overlap across phenotypes for variants that reached a high threshold of significance. Finally, we conducted a joint meta-analysis on the combined phenotype of IS or CAD. Corresponding analyses were performed restricted to the 2167 individuals with the ischemic large artery stroke (LAS) subtype. Results-Common variants associated with CAD at P<0.01 were associated with a significant excess risk for IS and for LAS and vice versa. Among the 42 known genome-wide significant loci for CAD, 3 and 5 loci were significantly associated with IS and LAS, respectively. In the joint meta-analyses, 15 loci passed genome-wide significance (P<5<i>x</i>10<sup>-8</sup>) for the combined phenotype of IS or CAD and 17 loci passed genome-wide significance for LAS or CAD. Because these loci had prior evidence for genome-wide significance for CAD, we specifically analyzed the respective signals for IS and LAS and found evidence for association at chr12q24/SH2B3 (P<sub>IS</sub>=1.62<i>x</i>10<sup>-7</sup>) and ABO (P<sub>IS</sub>=2.6<i>x</i>10<sup>-4</sup>), as well as at HDAC9 (P<sub>LAS</sub>=2.32<i>x</i>10-12), 9p21 (P<sub>LAS</sub>=3.70<i>x</i>10<sup>-6</sup>), RAI1-PEMT-RASD1 (P<sub>LAS</sub>=2.69<i>x</i>10<sup>-5</sup>), EDNRA (P<sub>LAS</sub>=7.29<i>x</i>10<sup>-4</sup>), and CYP17A1-CNNM2-NT5C2 (P<sub>LAS</sub>=4.9<i>x</i>10<sup>-4</sup>). Conclusions-Our results demonstrate substantial overlap in the genetic risk of IS and particularly the LAS subtype with CAD
