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Comparative Study
. 2010 Jul;27(7):1518-29.
doi: 10.1093/molbev/msq030. Epub 2010 Jan 29.

Haplotype structure and divergence at human and chimpanzee serotonin transporter and receptor genes: implications for behavioral disorder association analyses

Affiliations
Comparative Study

Haplotype structure and divergence at human and chimpanzee serotonin transporter and receptor genes: implications for behavioral disorder association analyses

Katrina G Claw et al. Mol Biol Evol. 2010 Jul.

Abstract

Genetic variation in the human serotonin system has long-been studied because of its functional consequences and links to various behavior-related disorders and it being routinely targeted in research and development for drug therapy. However, aside from clinical studies, little is known about this genetic diversity and how it differs within and between human populations with respect to haplotype structure, which can greatly impact phenotype association studies. In addition, no evolutionary approach among humans and other primates has examined how long- and short-term selective pressures explain existing serotonin variation. Here, we examine DNA sequence variation in natural population samples of 192 human and 40 chimpanzee chromosome sequences for the most commonly implicated approximately 38-kb serotonin transporter (SLC6A4) and approximately 63-kb serotonin 2A receptor (HTR2A) genes. Our comparative population genetic analyses find significant linkage disequilibrium associated with functionally relevant variants in humans, as well as geographic variation for these haplotypes, at both loci. In addition, although amino acid divergence is consistent with purifying selection, promoter and untranslated regions exhibit significantly high divergence in both species lineages. These evolutionary analyses imply that the serotonin system may have accumulated significant regulatory variation over both recent and ancient periods of time in both humans and chimpanzees. We discuss the implications of this variation for disease association studies and for the evolution of behavior-related phenotypes during the divergence of humans and our closest primate relatives.

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Figures

F<sc>IG</sc>. 1.
FIG. 1.
Gene diagrams for the (a) ∼63-kb HTR2A locus and (b) ∼38-kb SLC6A4 locus (with promoter “LPR” and intron 2 “VNTR” variants). Black boxes denote amino acid coding exons, white boxes denote UTRs, and striped boxes denote functionally identified promoter regions. SNP numbering is with respect to the beginning of amino acid translation. Genes are to scale (except where noted with collapsed distances in kb), and only regions for which data were collected are shown. Significant pairwise associations (filled boxes) among informative variants in 192 human (>5% in frequency) and 40 chimpanzee (>12% in frequency) chromosome sequences are above and below gene diagrams, respectively (see Materials and Methods and Results for more details).
F<sc>IG</sc>. 2.
FIG. 2.
Histogram plot for HTR2A −1438A/102T, SLC6A4 promoter LPR-S, SLC6A4 intron 2 VNTR 12-repeat, and SLC6A4 LPR-S/12-repeat/23966G haplotype frequencies, for each of the 10 human population samples (see Materials and Methods for abbreviations), as well as the overall global sample of 192 human chromosome sequences.

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