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首页> 外文期刊>The pharmacogenomics journal >Further evidence for association of the RGS2 gene with antipsychotic-induced parkinsonism: protective role of a functional polymorphism in the 3'-untranslated region.
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Further evidence for association of the RGS2 gene with antipsychotic-induced parkinsonism: protective role of a functional polymorphism in the 3'-untranslated region.

机译:RGS2基因与抗精神病药物诱发的帕金森氏症相关的进一步证据:功能性多态性在3'非翻译区的保护作用。

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摘要

RGS2 (regulator of G-protein signaling 2) modulates dopamine receptor signal transduction. Functional variants in the gene may influence susceptibility to extrapyramidal symptoms (EPS) induced by antipsychotic drugs. To further investigate our previous report of association of the RGS2 gene with susceptibility to antipsychotic-induced EPS, we performed a replication study. EPS were rated in 184 US patients with schizophrenia (115 African Americans, 69 Caucasian) treated for at least a month with typical antipsychotic drugs (n=45), risperidone (n=46), olanzapine (n=50) or clozapine (n=43). Six single nucleotide polymorphisms (SNPs) within or flanking RGS2 were genotyped (rs1933695, rs2179652, rs2746073, rs4606, rs1819741 and rs1152746). Odds ratios (ORs) and 95% confidence intervals (CIs) were calculated by logistic regression. Our results indicate association of SNP rs4606 with antipsychotic-induced parkinsonism (AIP), as measured by the Simpson Angus scale, in the overall sample and in the African-American subsample, the G (minor) allele having a protective effect. ORs for AIP among rs4606 G-allele carriers were 0.23 (95% CI 0.10-0.54, P=0.001) in the overall sample, and 0.20 (0.07-0.57, P=0.003) in the African-American subsample. In the previously studied Israeli sample the OR was 0.31 (0.11-0.84, P=0.02). We completely sequenced the RGS2 gene in nine patients with AIP and nine patients without, from the Israeli sample. No common coding polymorphisms or additional regulatory variants were revealed, suggesting that association of the rs4606 C/G polymorphism with AIP is biologically meaningful and not a consequence of linkage disequilibrium with another functional variant. Taken together, the findings of the current study support the association of RGS2 with AIP and focus on a possible protective effect of the minor G allele of SNP rs4606. This SNP is located in the 3'-regulatory region of the gene, and is known to influence RGS2 mRNA levels and protein expression.
机译:RGS2(G蛋白信号传导2的调节剂)调节多巴胺受体信号转导。该基因的功能变异可能会影响抗精神病药诱发的锥体外系症状(EPS)的易感性。为了进一步研究我们先前关于RGS2基因与抗精神病药物诱发的EPS易感性相关的报道,我们进行了一项复制研究。对184名美国精神分裂症患者(115名非洲裔美国人,69名白种人)的EPS进行了评估,这些患者使用典型的抗精神病药物(n = 45),利培酮(n = 46),olanzapine(n = 50)或clozapine(n = 43)。对RGS2内部或侧翼的六个单核苷酸多态性(SNP)进行基因分型(rs1933695,rs2179652,rs2746073,rs4606,rs1819741和rs1152746)。通过逻辑回归计算赔率(OR)和95%置信区间(CI)。我们的结果表明,在整个样本和非裔美国人子样本中,SNP rs4606与抗精神病药物致帕金森病(AIP)的关系(通过辛普森·安格斯量表进行了测量)在G(次要)等位基因具有保护作用。 rs4606 G等位基因携带者中AIP的OR总体样本为0.23(95%CI 0.10-0.54,P = 0.001),非裔美国人子样本为0.20(0.07-0.57,P = 0.003)。在先前研究的以色列样本中,OR为0.31(0.11-0.84,P = 0.02)。我们从以色列样本中对9例AIP患者和9例非AIP患者进行了RGS2基因的完全测序。没有发现常见的编码多态性或其他调控变异,这表明rs4606 C / G多态性与AIP的关联具有生物学意义,而不是与另一个功能性变异连锁不平衡的结果。两者合计,当前研究的结果支持RGS2与AIP的关联,并集中于SNP rs4606的次要G等位基因的可能的保护作用。该SNP位于基因的3'调节区,已知会影响RGS2 mRNA水平和蛋白质表达。

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