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基于基因的分析表明,烟碱型乙酰胆碱受体β1亚基(CHRNB1)和M1毒蕈碱型乙酰胆碱受体(CHRM1)与尼古丁依赖易感性有关。

Gene-based analysis suggests association of the nicotinic acetylcholine receptor beta1 subunit (CHRNB1) and M1 muscarinic acetylcholine receptor (CHRM1) with vulnerability for nicotine dependence.

作者信息

Lou Xiang-Yang, Ma Jennie Z, Payne Thomas J, Beuten Joke, Crew Karen M, Li Ming D

机构信息

Department of Psychiatric Medicine, University of Virginia, 1670 Discovery Drive, Suite 101, Charlottesville, VA 22911, USA.

出版信息

Hum Genet. 2006 Oct;120(3):381-9. doi: 10.1007/s00439-006-0229-7. Epub 2006 Jul 28.

DOI:10.1007/s00439-006-0229-7
PMID:16874522
Abstract

Based on our previously identified linkage regions for nicotine dependence (ND), we selected six and five single nucleotide polymorphisms (SNPs) in the muscarinic cholinergic receptor subtype M1 (CHRM1) and nicotinic cholinergic receptor beta1 (CHRNB1), respectively, to determine the association of the two genes with ND in a total of 2,037 subjects from 602 nuclear families of either African-American (AA) or European-American (EA) origin. Individual SNP- and/or haplotype-based analyses indicated that the CHRNB1 was significantly associated with ND, which was assessed by smoking quantity (SQ), the Heaviness of Smoking Index (HSI), and the Fagerström Test for ND (FTND), in both ethnic samples. The association of rs2302763 in the CHRNB1 was significant with adjusted SQ in the EA sample after correction for multiple testing (P=0.013). Haplotype A-T-A formed by SNPs rs2302765, rs2302762, and rs9217 in the CHRNB1 was significantly associated with the high risk allele for all the three ND measures (minimum P=0.009, 0.006, and 0.008 for SQ, HSI and FTND, respectively) in the AA sample while haplotype A-T-A formed by rs2302765, rs2302763, and rs9217 was significantly positively associated with ND (minimum P=0.005, 0.016, and 0.016 for SQ, HSI and FTND, respectively) in the EA sample. The CHRM1 exhibited significant protective associations of haplotype C-C-A-T-G-G formed by all six SNPs of this gene with at least one ND measure in the AA sample after Bonferroni correction (minimum P=0.008, 0.013, and 0.009 for SQ, HSI and FTND, respectively), but no significant association was found in the EA sample. The significant associations, together with their location of linked region to ND, suggest that the CHRNB1 and CHRM1 are likely candidates for further investigation.

摘要

基于我们之前确定的尼古丁依赖(ND)连锁区域,我们分别在毒蕈碱型胆碱能受体M1亚型(CHRM1)和烟碱型胆碱能受体β1(CHRNB1)中选择了6个和5个单核苷酸多态性(SNP),以确定这两个基因与来自602个非裔美国人(AA)或欧裔美国人(EA)核心家庭的2037名受试者的ND之间的关联。基于单个SNP和/或单倍型的分析表明,在两个种族样本中,CHRNB1与ND显著相关,ND通过吸烟量(SQ)、吸烟强度指数(HSI)和尼古丁依赖的Fagerström测试(FTND)进行评估。在多重检验校正后,CHRNB1中rs2302763与EA样本中经调整的SQ显著相关(P = 0.013)。CHRNB1中由SNP rs2302765、rs2302762和rs9217形成的单倍型A-T-A与AA样本中所有三项ND测量指标的高风险等位基因显著相关(SQ、HSI和FTND的最小P值分别为0.009、0.006和0.008),而由rs2302765、rs2302763和rs9217形成的单倍型A-T-A与EA样本中的ND显著正相关(SQ、HSI和FTND的最小P值分别为0.005、0.016和0.016)。在Bonferroni校正后,CHRM1中由该基因的所有6个SNP形成的单倍型C-C-A-T-G-G与AA样本中至少一项ND测量指标表现出显著的保护关联(SQ、HSI和FTND的最小P值分别为0.008、0.013和0.009),但在EA样本中未发现显著关联。这些显著关联及其与ND连锁区域的位置表明,CHRNB1和CHRM1可能是进一步研究的候选基因。

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