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首页> 外文期刊>European neuropsychopharmacology: the journal of the European College of Neuropsychopharmacology >Searching for functional SNPs or rare variants in exonic regions of DRD3 in risperidone-treated patients.
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Searching for functional SNPs or rare variants in exonic regions of DRD3 in risperidone-treated patients.

机译:在利培酮治疗的患者中寻找DRD3外显子区域的功能性SNP或罕见变体。

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摘要

Previously one intronic DRD3 SNP, rs167771, was associated with risperidone-induced extrapyramidal side-effects (EPS). The aim of the present study was to search hitherto unidentified common functional variants or rare variants, in DRD3 associated with risperidone-induced EPS. 126 subjects treated with risperidone participated in this study. We sequenced the seven exons of DRD3. After sequencing we localized five dbSNPs and four new rare variants. None of the dSNPs or rare variants seems to be functional after bioinformatics analysis. Our results suggest that, rather than exonic regions, regulatory regions and introns could be related to the associations reported for DRD3 and the incidence of locomotor side-effects.
机译:以前,一个内含子DRD3 SNP rs167771与利培酮诱导的锥体外系副作用(EPS)相关。本研究的目的是在与利培酮诱导的EPS相关的DRD3中寻找迄今尚未鉴定的常见功能变体或稀有变体。利培酮治疗的126名受试者参加了这项研究。我们对DRD3的七个外显子进行了测序。测序后,我们定位了五个dbSNP和四个新的罕见变体。经过生物信息学分析后,dSNP或稀有变异均无功能。我们的研究结果表明,调控区域和内含子可能与DRC3的关联性以及运动性副作用的发生率有关,而不是与外显子区域有关。

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