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人类P2Y2受体多态性:两种等位基因变体的鉴定与药理学特性分析

Human P2Y2 receptor polymorphism: identification and pharmacological characterization of two allelic variants.

作者信息

Janssens R, Paindavoine P, Parmentier M, Boeynaems J M

机构信息

Institute of Interdisciplinary Research, School of Medicine, Université Libre de Bruxelles, Belgium.

出版信息

Br J Pharmacol. 1999 Jun;127(3):709-16. doi: 10.1038/sj.bjp.0702619.

Abstract
  1. In the process of cloning the human P2Y2 receptor in order to establish 1321N1 cell lines expressing this receptor, we detected a gene polymorphism characterized by an arginine 334 to cysteine 334 transition. 2. The frequency distribution of the polymorphism was studied in a European population. We observed that 66% of the tested persons are homozygotes R/R, 29% are heterozygotes R/C and 5% are homozygotes C/C. The frequency of the R allele was 0.8 versus 0.2 for the C allele. 3. We stably expressed each form of the human P2Y2 receptor into 1321N1 cells and isolated clones by limiting dilution. The effects of nucleotides and antagonists on inositol trisphosphate accumulation and cyclic AMP formation were compared between the two cell lines. 4. The time-courses of inositol trisphosphate accumulation as well as concentration-response curves characterizing the effects of UTP, ATP, AP4A and ATP gamma S were mostly similar, except for slight kinetic differences (slower time-course with the 334C form). 5. The sensitivity to pertussis toxin of inositol trisphosphates accumulation was critically dependent on the agonist concentration and stimulation duration, suggesting the involvement of a Gi.0 protein during the early stimulation by low nucleotide concentrations. No inhibition of cyclic AMP accumulation could be detected. These properties were observed with both polymorphic receptors.
摘要
  1. 在克隆人P2Y2受体以建立表达该受体的1321N1细胞系的过程中,我们检测到一种基因多态性,其特征为精氨酸334向半胱氨酸334的转变。2. 研究了该多态性在欧洲人群中的频率分布。我们观察到,66%的受测者为纯合子R/R,29%为杂合子R/C,5%为纯合子C/C。R等位基因的频率为0.8,而C等位基因的频率为0.2。3. 我们将人P2Y2受体的每种形式稳定表达于1321N1细胞中,并通过有限稀释法分离克隆。比较了两种细胞系中核苷酸和拮抗剂对肌醇三磷酸积累和环磷酸腺苷形成的影响。4. 肌醇三磷酸积累的时间进程以及表征UTP、ATP、AP4A和ATPγS作用的浓度-反应曲线大多相似,只是存在轻微的动力学差异(334C形式的时间进程较慢)。5. 肌醇三磷酸积累对百日咳毒素的敏感性严重依赖于激动剂浓度和刺激持续时间,这表明在低核苷酸浓度的早期刺激过程中涉及Gi.0蛋白。未检测到环磷酸腺苷积累的抑制作用。两种多态性受体均观察到这些特性。

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