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首页> 外文期刊>Human Molecular Genetics >Fine mapping of a linkage region on chromosome 17p13 reveals that GABARAP and DLG4 are associated with vulnerability to nicotine dependence in European-Americans.
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Fine mapping of a linkage region on chromosome 17p13 reveals that GABARAP and DLG4 are associated with vulnerability to nicotine dependence in European-Americans.

机译:染色体17p13上一个连锁区域的精细定位揭示了GABARAP和DLG4与欧美人对尼古丁依赖的脆弱性有关。

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A two-stage association study was conducted targeting a genomic region on chromosome 17p13 that we reported likely to harbor susceptibility gene(s) for nicotine dependence (ND). Participants were 2037 subjects from 602 nuclear families of either African-American (AA) or European-American (EA) origin from our Mid-South Tobacco Family (MSTF) cohort. We first examined 10 single nucleotide polymorphisms (SNPs) in six genes within the targeted region of about 90 kb to determine which SNP/gene was associated with ND, assessed by smoking quantity (SQ), the heaviness of smoking index (HSI) and the Fagerstrom Test for ND (FTND). Individual SNP analysis revealed that SNPs rs17710 and rs222843 in GABA(A) receptor-associated protein (GABARAP) exhibited a significant association with at least one age- and gender-adjusted ND measure in the EA sample and rs222843 remained significant with the FTND after correction for multiple testing (P = 0.009). Although no SNP in DLG4 was significantly associated with ND, we founda G-G haplotype with a frequency of 14.2% formed by SNPs rs2242449 and rs507506 within the gene that showed significant inverse associations with all three ND measures [P = 0.003, 0.015 and 0.024, for SQ (defined as the number of cigarettes smoked per day), HSI and FTND, respectively]. We also found an A-A haplotype with a frequency of 8.8% formed by SNPs rs17710 and rs222843 in GABARAP, which revealed significant associations with all three ND measures (P = 0.006, 0.019 and 0.024, for SQ, HSI and FTND, respectively). To confirm these findings with a better coverage of GABARAP and DLG4, we conducted a second-stage association analysis by genotyping four more SNPs for GABARAP and nine more for DLG4 on the same set of samples. Our results from the second stage of individual SNP- and/or haplotype-based association analysis supported our finding of significant association of the DLG4 gene with ND. No significant association of GABARAP or DLG4 with ND was detected in the AA sample. Further, by comparing the linkage signal before and after adjustment for the SNPs of GABARAP and DLG4, we found that inclusion of the SNPs of the two genes as covariates largely reduced the linkage signal in the EA sample, but kept nearly unchanged in the AA sample. Taken together, our two-stage association analysis and linkage analysis results indicate that the GABARAP and DLG4 genes are involved in the etiology of ND in EA smokers. Further investigation of neurobiological mechanisms of the two genes in the etiology of ND is thus warranted.
机译:针对17p13染色体上的一个基因组区域进行了两阶段关联研究,我们报道了该基因区域可能具有尼古丁依赖性(ND)易感性基因。参与者是来自我们中南烟草家族(MSTF)队列的602个非裔美国人(AA)或欧洲裔美国人(EA)核心家庭的2037名受试者。我们首先检查了约90 kb靶区域内六个基因中的10个单核苷酸多态性(SNP),以确定哪个SNP /基因与ND相关,并通过吸烟量(SQ),吸烟指数(HSI)和重度进行评估。 Fagerstrom ND测试(FTND)。单独的SNP分析显示,GABA(A)受体相关蛋白(GABARAP)中的SNP rs17710和rs222843与EA样品中至少一项经过年龄和性别调整的ND量度显示显着相关,并且校正后rs222843与FTND仍然显着用于多次测试(P = 0.009)。尽管DLG4中没有SNP与ND显着相关,但我们发现基因中的SNP rs2242449和rs507506形成的GG单倍型的频率为14.2%,与所有三种ND度量均显示出显着的负相关[P = 0.003、0.015和0.024,对于SQ(定义为每天吸烟的数量),HSI和FTND]。我们还发现了由GABARAP中的SNP rs17710和rs222843形成的A-A单倍型,其频率为8.8%,这揭示了与所有三个ND度量的显着相关性(SQ,HSI和FTND分别为P = 0.006、0.019和0.024)。为了更好地覆盖GABARAP和DLG4,以证实这些发现,我们通过对同一组样本中GABARAP的另外四个SNP和DLG4的另外九个SNP进行基因分型,进行了第二阶段关联分析。我们基于基于SNP和/或单倍型的个体关联分析第二阶段的结果支持了我们发现DLG4基因与ND的显着关联。在AA样品中未检测到GABARAP或DLG4与ND的显着关联。此外,通过比较调整GABARAP和DLG4的SNP前后的连锁信号,我们发现以协变量的形式包含两个基因的SNP大大减少了EA样品中的连锁信号,但在AA样品中几乎保持不变。综上所述,我们的两阶段关联分析和连锁分析结果表明,GABARAP和DLG4基因参与了EA吸烟者ND的病因。因此,有必要在ND病因中进一步研究这两个基因的神经生物学机制。

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