A common polymorphism in serotonin receptor 1B mRNA moderates regulation by miR-96 and associates with aggressive human behaviors

被引:0
作者
K P Jensen
J Covault
T S Conner
H Tennen
H R Kranzler
H M Furneaux
机构
[1] Graduate Program in Molecular Biology and Biochemistry,Department of Molecular
[2] Microbial and Structural Biology,Department of Psychiatry
[3] University of Connecticut Health Center,undefined
[4] Alcohol Research Center,undefined
[5] University of Connecticut School of Medicine,undefined
来源
Molecular Psychiatry | 2009年 / 14卷
关键词
microRNA; polymorphism; behavior; aggression; human;
D O I
暂无
中图分类号
学科分类号
摘要
Non-coding regulatory elements can transduce the human genome's response to environmental stimuli. Thus, there is a possibility that variation in non-coding regulatory elements may underlie some of the diversity in human behavior. However, this idea has remained largely untested due to the difficulty in accurately identifying regulatory elements in the 98% of the human genome that does not encode protein. The recent recognition that small trans-acting RNAs anneal to mRNA and regulate gene expression provides a means to identify and test such variants. Here, we show that microRNA-directed silencing of mRNA can be attenuated by a common human polymorphism. We have identified an element (A-element) within serotonin receptor 1B (HTR1B) mRNA that confers repression by miR-96. The repressive activity of this element is attenuated by a common human variant (G-element) that disrupts a nucleotide critical for its interaction with miR-96. Because deletion of the HTR1B gene leads to an aggressive phenotype in mice, we hypothesized an association between the A/G polymorphism and aggressive phenotypes in a sample of 359 college students. As predicted, individuals homozygous for the ancestral A-element reported more conduct-disorder behaviors than individuals with the G-element. Our studies suggest that such functional variants may be common and may help to refine the search for genes involved in complex behavioral disorders.
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页码:381 / 389
页数:8
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