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复杂的启动子和编码区β2 - 肾上腺素能受体单倍型改变受体表达并预测体内反应性。

Complex promoter and coding region beta 2-adrenergic receptor haplotypes alter receptor expression and predict in vivo responsiveness.

作者信息

Drysdale C M, McGraw D W, Stack C B, Stephens J C, Judson R S, Nandabalan K, Arnold K, Ruano G, Liggett S B

机构信息

Genaissance Pharmaceuticals, Inc., New Haven, CT 06511, USA.

出版信息

Proc Natl Acad Sci U S A. 2000 Sep 12;97(19):10483-8. doi: 10.1073/pnas.97.19.10483.

DOI:10.1073/pnas.97.19.10483
PMID:10984540
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC27050/
Abstract

The human beta(2)-adrenergic receptor gene has multiple single-nucleotide polymorphisms (SNPs), but the relevance of chromosomally phased SNPs (haplotypes) is not known. The phylogeny and the in vitro and in vivo consequences of variations in the 5' upstream and ORF were delineated in a multiethnic reference population and an asthmatic cohort. Thirteen SNPs were found organized into 12 haplotypes out of the theoretically possible 8,192 combinations. Deep divergence in the distribution of some haplotypes was noted in Caucasian, African-American, Asian, and Hispanic-Latino ethnic groups with >20-fold differences among the frequencies of the four major haplotypes. The relevance of the five most common beta(2)-adrenergic receptor haplotype pairs was determined in vivo by assessing the bronchodilator response to beta agonist in asthmatics. Mean responses by haplotype pair varied by >2-fold, and response was significantly related to the haplotype pair (P = 0.007) but not to individual SNPs. Expression vectors representing two of the haplotypes differing at eight of the SNP loci and associated with divergent in vivo responsiveness to agonist were used to transfect HEK293 cells. beta(2)-adrenergic receptor mRNA levels and receptor density in cells transfected with the haplotype associated with the greater physiologic response were approximately 50% greater than those transfected with the lower response haplotype. The results indicate that the unique interactions of multiple SNPs within a haplotype ultimately can affect biologic and therapeutic phenotype and that individual SNPs may have poor predictive power as pharmacogenetic loci.

摘要

人类β₂ - 肾上腺素能受体基因存在多个单核苷酸多态性(SNP),但染色体定相SNP(单倍型)的相关性尚不清楚。在一个多民族参考人群和一个哮喘队列中,描绘了5'上游和开放阅读框变异的系统发育以及体外和体内后果。在理论上可能的8192种组合中,发现13个SNP组成了12种单倍型。在高加索人、非裔美国人、亚洲人和西班牙裔 - 拉丁裔族群中,注意到某些单倍型分布存在深度差异,四种主要单倍型的频率差异超过20倍。通过评估哮喘患者对β激动剂的支气管扩张反应,在体内确定了五种最常见的β₂ - 肾上腺素能受体单倍型对的相关性。单倍型对的平均反应差异超过2倍,且反应与单倍型对显著相关(P = 0.007),但与单个SNP无关。使用代表在8个SNP位点不同且与体内对激动剂的不同反应相关的两种单倍型的表达载体转染HEK293细胞。转染与更大生理反应相关单倍型的细胞中,β₂ - 肾上腺素能受体mRNA水平和受体密度比转染反应较低单倍型的细胞高约50%。结果表明,单倍型内多个SNP的独特相互作用最终可影响生物学和治疗表型,且单个SNP作为药物遗传学位点的预测能力可能较差。

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