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The Differential Effect of NAT2 Variant Alleles Permits Refinement in Phenotype Inference and Identifies a Very Slow Acetylation Genotype

机译:NaT2变异等位基因的不同影响许可证细化表型推理和标识非常慢乙酰化基因型

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摘要

Indirect evidences suggest that acetylation phenotype categories are heterogeneous and that subcategories, related to specific NAT2 variant alleles might exist. We analyzed the in vivo acetylation phenotype and genotype in 504 north-American subjects of Caucasian origin. The analyses of the SNPs rs1801280 and rs1799930 allowed the discrimination of five categories with different acetylation status within the study population. These categories are related to the distinct effect of NAT2 alleles on the acetylation status in vivo and to the occurrence of a gene-dose effect. These five phenotype categories, from higher to lower acetylation capacity, correspond to the genotypes NAT2*4/*4, NAT2*4/*5 or *4/*6, NAT2*5/*5, NAT2*5/*6 and NAT2*6/*6 (p≤0.001 for all comparisons). The NAT2*6/*6 genotype correspond to a phenotype category of very-slow acetylators. The refinement in phenotype prediction may help to identify risks associated to phenotype subcategories, and warrants the re-analysis of previous studies that may have overlooked phenotype subcategory-specific risks.
机译:间接证据表明,乙酰化表型类别是异质的,并且可能存在与特定NAT2变异等位基因相关的子类别。我们分析了白种人的504名北美受试者的体内乙酰化表型和基因型。通过对SNP rs1801280和rs1799930的分析,可以区分研究人群中五种乙酰化状态不同的类别。这些类别与NAT2等位基因对体内乙酰化状态的独特作用以及基因剂量效应的发生有关。从较高到较低的乙酰化能力,这五个表型类别分别对应于NAT2 * 4 / * 4,NAT2 * 4 / * 5或* 4 / * 6,NAT2 * 5 / * 5,NAT2 * 5 / * 6和NAT2 * 6 / * 6(对于所有比较,p≤0.001)。 NAT2 * 6 / * 6基因型对应于极慢的乙酰化酶的表型类别。表型预测的改进可以帮助识别与表型亚类相关的风险,并保证重新分析以前可能忽略了表型亚类特定风险的研究。

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