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利用一种针对多等位基因标记的新型分组方法,对白介素-1基因簇中的连锁不平衡进行分析。

An analysis of linkage disequilibrium in the interleukin-1 gene cluster, using a novel grouping method for multiallelic markers.

作者信息

Cox A, Camp N J, Nicklin M J, di Giovine F S, Duff G W

机构信息

Division of Molecular and Genetic Medicine, University of Sheffield, Sheffield, United Kingdom.

出版信息

Am J Hum Genet. 1998 May;62(5):1180-8. doi: 10.1086/301817.

Abstract

In population- and family-based association studies, it is useful to have some knowledge of the patterns of linkage disequilibrium that exist between markers in candidate regions. When such studies are carried out with multiallelic markers, it is often convenient to group the alleles into a biallelic system, for analysis. In this study, we specifically examined the interleukin-1 (IL-1) gene cluster on chromosome 2, a region containing candidates for many inflammatory and autoimmune disorders. Data were collected on eight markers, four of which were multiallelic. Using these data, we investigated the effect of three allele-grouping strategies, including a novel method, on the detection of linkage disequilibrium. The novel approach, termed the "delta method," measures the deviation from the expected haplotype frequencies under linkage equilibrium, for each allelic combination. This information is then used to group the alleles, in an attempt to avoid the grouping together of alleles at one locus that are in opposite disequilibrium with the same allele at the second locus. The estimate haplotype frequencies (EH) program was used to estimate haplotype frequencies and the disequilibrium measure. In our data it was found that the delta method compared well with the other two strategies. Using this method, we found that there was a reasonable correlation between disequilibrium and physical distance in the region (r=-.540, P=.001, one-tailed). We also identified a common, eight-locus haplotype of the IL-1 gene cluster.

摘要

在基于人群和家庭的关联研究中,了解候选区域内标记之间存在的连锁不平衡模式是很有用的。当使用多等位基因标记进行此类研究时,为了便于分析,通常将等位基因分组为双等位基因系统。在本研究中,我们专门研究了2号染色体上的白细胞介素-1(IL-1)基因簇,该区域包含许多炎症和自身免疫性疾病的候选基因。收集了8个标记的数据,其中4个是多等位基因的。利用这些数据,我们研究了三种等位基因分组策略(包括一种新方法)对连锁不平衡检测的影响。这种新方法称为“δ方法”,它测量每个等位基因组合在连锁平衡下与预期单倍型频率的偏差。然后利用这些信息对等位基因进行分组,以避免将一个位点上与第二个位点上相同等位基因处于相反不平衡状态的等位基因组合在一起。使用估计单倍型频率(EH)程序来估计单倍型频率和不平衡度量。在我们的数据中发现,δ方法与其他两种策略相比效果良好。使用这种方法,我们发现该区域不平衡与物理距离之间存在合理的相关性(r = -0.540,P = 0.001,单尾)。我们还鉴定出了IL-1基因簇的一种常见的8位点单倍型。

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