Bernstein Jonathan A, Zhang Ge, Jin Li, Abbott Carol, Nebert Daniel W
University of Cincinnati College of Medicine, Department of Internal Medicine, Division of Immunology/Allergy Section, University of Cincinnati College of Medicine, Cincinnati, Ohio 45267-0053, USA.
J Asthma. 2008 May;45(4):287-92. doi: 10.1080/02770900701867579.
We sought a genotype-phenotype association: between single-nucleotide polymorphisms (SNPs) in olfactory receptor (OR) genes from the two largest OR gene clusters and odor-triggered nonallergic vasomotor rhinitis (nVMR). In the initial pedigree screen, using transmission disequilibrium test (TDT) analysis, six SNPs showed "significant" p-values between 0.0449 and 0.0043. In a second case-control population, the previously identified six SNPs did not re-emerge, whereas four new SNPs showed p-values between 0.0490 and 0.0001. Combining both studies, none of the SNPs in the TDT analysis survived the Bonferroni correction. In the population study, one SNP showed an empirical p-value of 0.0066 by shuffling cases and controls with 10(5) replicates; however, the p-value for this SNP was 0.83 in the pedigree study. This study emphasizes that underpowered studies having p-values between < 0.05 and 0.0001 should be regarded as inconclusive and require further replication before concluding the study is "informative." However, we believe that our hypothesis that an association between OR genotypes and the nVMR phenotype remains feasible. Future studies using either a genomewide association study of all OR gene-pseudogene regions throughout the genome--at the current recommended density of 2.5 to 5 kb per tag SNP--or studies incorporating microarray analyses of the entire "OR genome" in well-characterized nVMR patients are required.
即来自两个最大嗅觉受体(OR)基因簇的单核苷酸多态性(SNP)与气味诱发的非过敏性血管运动性鼻炎(nVMR)之间的关联。在初始家系筛查中,使用传递不平衡检验(TDT)分析,6个SNP显示出介于0.0449至0.0043之间的“显著”P值。在第二个病例对照人群中,先前鉴定出的6个SNP未再次出现,而4个新的SNP显示出介于0.0490至0.0001之间的P值。综合两项研究,TDT分析中的SNP无一通过Bonferroni校正。在人群研究中,通过对病例和对照进行10⁵次重复洗牌,一个SNP显示出经验性P值为0.0066;然而,该SNP在系谱研究中的P值为0.83。这项研究强调,P值介于<0.05至0.0001之间且样本量不足的研究应被视为无定论,在得出该研究“有参考价值”的结论之前需要进一步重复验证。然而,我们认为我们关于OR基因型与nVMR表型之间存在关联的假设仍然可行。未来需要开展以下研究:要么对整个基因组中所有OR基因 - 假基因区域进行全基因组关联研究——按照目前推荐的每个标签SNP 2.5至5 kb的密度——要么对特征明确的nVMR患者进行包含整个“OR基因组”微阵列分析的研究。