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The C/C genotype of the C957T polymorphism of the dopamine D2 receptor (DRD2) is associated with schizophrenia

机译:多巴胺D2受体(DRD2)C957T多态性的C / C基因型与精神分裂症相关

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摘要

The T allele of the human dopamine D2 receptor (DRD2) gene C957T polymorphism is associated with reduced mRNA translation and stability. This results in decreased dopamine induced DRD2 upregulation and decreased in-vivo D2 dopamine binding. Conversely, the C allele of the C957T polymorphism is not associated with such changes in mRNA leading to increased DRD2 expression. PET and post-mortem binding studies show that schizophrenia is often associated with increased DRD2 availability. We report that on the basis of comparing the frequencies of the C/C and T/T genotypes of 153 patients with schizophrenia and 148 controls that schizophrenia is associated with the C/C genotype. The C957T shows a population attributable risk for schizophrenia of 24% and an attributable risk in those with schizophrenia of 42%. Increased expression of D2 receptors associated with the C allele is likely to be important in the underlying pathophysiology of at least some forms of schizophrenia. Enhanced understanding of schizophrenia afforded by this finding may lead to advances in treatment and prevention.
机译:人多巴胺D2受体(DRD2)基因C957T多态性的T等位基因与减少的mRNA翻译和稳定性有关。这导致多巴胺诱导的DRD2上调减少,体内D2多巴胺结合减少。相反,C957T多态性的C等位基因与导致DRD2表达增加的mRNA改变无关。 PET和验尸结合研究表明,精神分裂症通常与DRD2可用性增加有关。我们报告的基础上比较153精神分裂症患者和148控件的精神分裂症的C / C和T / T基因型的频率与C / C基因型相关。 C957T显示,精神分裂症的人群归因风险为24%,精神分裂症人群的归因风险为42%。与C等位基因相关的D2受体表达的增加在至少某些形式的精神分裂症的潜在病理生理中可能很重要。该发现对精神分裂症的加深理解可能会导致治疗和预防方面的进步。

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