2011
DOI: 10.1038/ng.943
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Large-scale genome-wide association analysis of bipolar disorder identifies a new susceptibility locus near ODZ4

Abstract: We conducted a combined genome-wide association (GWAS) analysis of 7,481 individuals affected with bipolar disorder and 9,250 control individuals within the Psychiatric Genomewide Association Study Consortium Bipolar Disorder group (PGC-BD). We performed a replication study in which we tested 34 independent SNPs in 4,493 independent bipolar disorder cases and 42,542 independent controls and found strong evidence for replication. In the replication sample, 18 of 34 SNPs had P value < 0.05, and 31 of 34 SNPs had… Show more

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Cited by 1,254 publications
(848 citation statements)
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“…The majority of SNPs (n = 26) imputed with <10% missing data, but some SNPs had higher failure rates (Supporting Information Table S1). The allele frequencies of each SNP in all European ancestry subjects were close to those previously reported [Sklar et al, 2011] for Europeans (±0.022–0.032), and were similar for both directly observed and imputed SNPs (±0.031 and ±0.025, respectively) (Supporting Information Table S1).…”
Section: Methodssupporting
confidence: 88%
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“…The majority of SNPs (n = 26) imputed with <10% missing data, but some SNPs had higher failure rates (Supporting Information Table S1). The allele frequencies of each SNP in all European ancestry subjects were close to those previously reported [Sklar et al, 2011] for Europeans (±0.022–0.032), and were similar for both directly observed and imputed SNPs (±0.031 and ±0.025, respectively) (Supporting Information Table S1).…”
Section: Methodssupporting
confidence: 88%
“…We chose for genotyping 38 SNPs that were robustly implicated in bipolar disorder risk, on the basis of prior evidence of genetic association ( P  < 5 × 10 −5 ) from the PGC [Sklar et al, 2011]; two (rs3968, rs8006348) failed sassay design.…”
Section: Methodsmentioning
confidence: 99%
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