Polymorphisms in seizure 6-like gene are associated with bipolar disorder I: Evidence of geneXgender interaction

Background: Previous reports have suggested that there may be geneXgender interaction for bipolar disorder (BD)-associated genes/loci at 22q11-13. This study aimed to investigate the associations of SEZ6L genetic variants with bipolar disorder I (BD-I) and to examine gender-specific genetic associat...

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Published in:Journal of affective disorders 2013-02, Vol.145 (1), p.95-99
Main Authors: Xu, Chun, Mullersman, Jerald E, Wang, Liang, Bin Su, Brenda, Mao, ChunXiang, Posada, Yolanda, Camarillo, Cynthia, Mao, Yu, Escamilla, Michael A, Wang, Ke-Sheng
Format: Article
Language:English
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Summary:Background: Previous reports have suggested that there may be geneXgender interaction for bipolar disorder (BD)-associated genes/loci at 22q11-13. This study aimed to investigate the associations of SEZ6L genetic variants with bipolar disorder I (BD-I) and to examine gender-specific genetic associations. Methods: 605 BD-I Caucasian cases and 1034 controls were selected from the publicly available data of the Whole Genome Association Study of BD. To increase power, an additional 362 Caucasian controls were added to this study from the Genome-Wide Association Study of Schizophrenia. In total, 605 BD-I cases and 1396 controls (934 males and 1067 females) were available for genetic association analysis of 118 SNPs within the SEZ6L gene using PLINK software. Results: 16 SNPs showed significant gene x gender interactions influencing BD-I (P0.05). The SNP rs4822691 showed the strongest association with BD-I in the female sample (P=2.18X10-4) and the strongest geneXgender interaction in influencing BD-I (P=9.16X10-5). Limitations: The findings of this study need to be replicated in independent samples. Conclusions: This is the first demonstration that genetic variants in the SEZ6L gene are associated with BD-I in female patients and provides additional compelling evidence for genetic variation at 22q11-13 that influences BD-I risk. The present findings highlight the gene x gender interactions modifying BD-I susceptibility.
ISSN:0165-0327