Sequence variation and linkage disequilibrium in the GABA transporter-1 gene (SLC6A1) in five populations: implications for pharmacogenetic research

Rungnapa Hirunsatit,Jaakko Lappalainen,Risto Ilomäki,Henry R Kranzler,Pirkko Räsänen,Jennifer Listman,Joel Gelernter,Atapol Sughondhabirom,Essi Ilomäki,Thomas Kosten,Sookjaroen Tangwongchai,Apiwat Mutirangura,Nuntika Thavichachart,Robert Malison

doi:10.1186/1471-2156-8-71

Abstract

BackgroundGABA transporter-1 (GAT-1; genetic locus SLC6A1) is emerging as a novel target for treatment of neuropsychiatric disorders. To understand how population differences might influence strategies for pharmacogenetic studies, we identified patterns of genetic variation and linkage disequilibrium (LD) in SLC6A1 in five populations representing three continental groups.ResultsWe resequenced 12.4 kb of SLC6A1, including the promoters, exons and flanking intronic regions in African-American, Thai, Hmong, Finnish, and European-American subjects (total n = 40). LD in SLC6A1 was examined by genotyping 16 SNPs in larger samples. Sixty-three variants were identified through resequencing. Common population-specific variants were found in African-Americans, including a novel 21-bp promoter region variable number tandem repeat (VNTR), but no such variants were found in any of the other populations studied. Low levels of LD and the absence of major LD blocks were characteristic of all five populations. African-Americans had the highest genetic diversity. European-Americans and Finns did not differ in genetic diversity or LD patterns. Although the Hmong had the highest level of LD, our results suggest that a strategy based on the use of tag SNPs would not translate to a major improvement in genotyping efficiency.ConclusionOwing to the low level of LD and presence of recombination hotspots, SLC6A1 may be an example of a problematic gene for association and haplotype tagging-based genetic studies. The 21-bp promoter region VNTR polymorphism is a putatively functional candidate allele for studies focusing on variation in GAT-1 function in the African-American population.

Highlights

GABA transporter-1 (GAT-1; genetic locus SLC6A1) is emerging as a novel target for treatment of neuropsychiatric disorders
Functional studies focusing on understanding whether the short and long allele lead to differential expression of the GAT-1 protein are clearly warranted; these studies may help in elucidating whether the allele frequency discrepancy between African-Americans and other populations is due to genetic drift or selection
A comparable promoter region variable number tandem repeat (VNTR) polymorphism was described in the serotonin transporter gene, which is known to influence the expression of the gene [22]

Summary

Objectives

In anticipation of larger pharmacogenetic studies, we aimed to identify novel genetic variation and examine linkage disequilibrium in the SLC6A1 gene in five populations representing three major continental groups [European (EA and Finnish), African (AA) and Asian (Thai and Hmong)]. Our goal was to identify a set of haplotype tagging markers for studies focusing on response to GAT-1 inhibition. The goal of the present study was to comprehensively analyze sequence variation and linkage disequilibrium in the SLC6A1 gene in anticipation of larger pharmacogenetic studies of tiagabine and other GAT-1 inhibitors

Methods

Results

Discussion

Conclusion