OCT1 多态性与抗帕金森病药物使用者的反应和生存时间有关。
OCT1 polymorphism is associated with response and survival time in anti-Parkinsonian drug users.
机构信息
Department of Epidemiology, Erasmus MC, P.O. Box 2040, 3000 CA, Rotterdam, The Netherlands.
出版信息
Neurogenetics. 2011 Feb;12(1):79-82. doi: 10.1007/s10048-010-0254-5. Epub 2010 Aug 1.
Substrates for the Organic Cation Transporter 1, encoded by the SLC22A1 gene, are metformin, amantadine, pramipexole, and, possibly, levodopa. Recently, we identified that the rs622342 A > C polymorphism is associated with the HbA1c lowering effect in metformin users. In the Rotterdam Study, we associated this polymorphism with higher prescribed doses of all anti-Parkinsonian drugs. Between the first and fifth prescriptions for levodopa, for each minor rs622342 C allele, the prescribed doses were 0.34 defined daily dose higher (95% CI 0.064, 0.62; p=0.017). The mortality ratio after start of levodopa therapy was 1.47 times higher (95% CI 1.01, 2.13; p=0.045).
SLC22A1 基因编码的有机阳离子转运蛋白 1 的底物包括二甲双胍、金刚烷胺、普拉克索,可能还包括左旋多巴。最近,我们发现 rs622342A>C 多态性与二甲双胍使用者的 HbA1c 降低效果有关。在鹿特丹研究中,我们发现这种多态性与所有抗帕金森病药物的更高处方剂量有关。在左旋多巴的第一次和第五次处方之间,对于每个次要的 rs622342C 等位基因,处方剂量高出 0.34 个定义日剂量(95%CI 0.064,0.62;p=0.017)。左旋多巴治疗开始后的死亡率比值高 1.47 倍(95%CI 1.01,2.13;p=0.045)。
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