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Functional characterization of the human TPH2 5′ regulatory region: untranslated region and polymorphisms modulate gene expression in vitro

机译:人TPH2 5'调控区的功能表征:非翻译区和多态性调节体外基因表达

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摘要

Tryptophan hydroxylase-2 (TPH2) is a recently identified TPH isoform responsible for neuronal serotonin (5-HT) synthesis, and TPH2 polymorphisms are associated with a range of behavioral traits and psychiatric disorders. This study characterized cis-acting elements and three common polymorphisms (?703G/T, ?473T/A, and 90A/G) in the 5′ regulatory region of human TPH2 by using luciferase reporter assay, quantitative real-time PCR, and electrophoretic mobility shift assay (EMSA). The core promoter of human TPH2 was localized to the region between ?107 and +7, and the segment of +8 to +53 within the 5′-UTR was found to exert a potent inhibitory effect on gene expression at both transcriptional and post-transcriptional levels. In both RN46A and HEK-293 cell lines, the TTA (?703T/?473T/90A) haplotype of the three polymorphisms showed the lowest gene expression compared with other haplotypes, and the ?703G/T and ?473T/A polymorphisms tended to exert a synergic effect on gene expression dependent upon the sequence of the 5′-UTR. In RN46A, the 90A/G polymorphism significantly increased luciferase activity and mRNA level irrespective of the other two polymorphisms, while in HEK-293 cells the effect of 90A/G was dependent on the alleles at loci ?703 and ?473. EMSA showed that all the three polymorphisms potentially alter DNA–protein interactions, while the 90A/G polymorphism predictably alters the 5′-UTR secondary structure of mRNA and influences RNA–protein interactions. In conclusion, our present study demonstrates that both the 5′-UTR and common polymorphisms (especially the 90A/G) in the 5′ regulatory region of human TPH2 have a significant impact on gene expression.
机译:色氨酸羟化酶2(TPH2)是最近鉴定出的负责神经元5-羟色胺(5-HT)合成的TPH亚型,而TPH2多态性与一系列行为特征和精神疾病有关。这项研究通过萤光素酶报告基因分析,实时荧光定量PCR和电​​泳技术表征了人TPH2 5'调控区的顺式作用元件和三个常见的多态性(?703G / T,?473T / A和90A / G)。迁移率变动分析(EMSA)。人TPH2的核心启动子位于约107和+7之间,发现5'-UTR中+8至+53的片段在转录和转录后均对基因表达产生有效的抑制作用。转录水平。在RN46A和HEK-293细胞系中,三种多态性的TTA(?703T /?473T / 90A)单倍型与其他单倍型相比均显示出最低的基因表达,而?703G / T和?473T / A多态性倾向于取决于5'-UTR的序列对基因表达发挥协同作用。在RN46A中,无论其他两个多态性如何,90A / G多态性均显着增加了荧光素酶活性和mRNA水平,而在HEK-293细胞中,90A / G的作用取决于基因座?703和?473。 EMSA显示所有这三种多态性都可能改变DNA与蛋白质的相互作用,而90A / G多态性可预测地改变mRNA的5'-UTR二级结构并影响RNA-蛋白质的相互作用。总之,我们的研究表明,人TPH2 5'调控区中的5'-UTR和常见多态性(尤其是90A / G)均对基因表达产生重大影响。

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    《Human Genetics》 |2008年第6期|645-657|共13页
  • 作者单位

    New England Primate Research Center Division of Neurochemistry Harvard Medical School One Pine Hill Drive Southborough MA 01772–9102 USA;

    New England Primate Research Center Division of Neurochemistry Harvard Medical School One Pine Hill Drive Southborough MA 01772–9102 USA;

    New England Primate Research Center Division of Neurochemistry Harvard Medical School One Pine Hill Drive Southborough MA 01772–9102 USA;

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