Correcting for biases in affected sib-pair linkage analysis caused by uncertainty in sibling relationship

Correcting for biases in affected sib-pair linkage analysis caused by uncertainty in sibling relationship

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摘要 When there is uncertainty in sibling relationship,the classical affected sib-pair(ASP) linkage tests may be severely biased.This can happen,for example,if some of the half sib-pairs are mixed with full sib-pairs.The genomic control method has been used in association analysis to adjust for population structures.We show that the same idea can be applied to ASP linkage analysis with uncertainty in sibling relationship.Assuming that,in addition to the candidate marker,null markers that are unlinked to the disease locus are also genotyped,we may use the information on these loci to estimate the proportion of half sib-pairs and to correct for the bias and variance distortion caused by the heterogeneity of sibling relationship.Unlike in association studies,the null loci are not required to be matched with the candidate marker in allele frequency for ASP linkage analysis.This makes our approach flexible in selecting null markers.In our simulations,using a number of 30 or more null loci can effectively remove the bias and variance distortion.It is also shown that,even the null loci are weakly linked to the disease locus,the proposed method can also provide satisfactory correction. When there is uncertainty in sibling relationship, the classical affected sib-pair （ASP） linkage tests may be severely biased. This can happen, for example, if some of the half sib-pairs are mixed with full sib-pairs. The genomic control method has been used in association analysis to adjust for population structures. We show that the same idea can be applied to ASP linkage analysis with uncertainty in sibling relationship. Assuming that, in addition to the candidate marker, null markers that are unlinked to the disease locus are also genotyped~ we may use the information on these loci to estimate the proportion of half sib-pairs and to correct for the bias and variance distortion caused by the heterogeneity of sibling relationship. Unlike in association studies, the null loci are not required to be matched with the candidate marker in allele frequency for ASP linkage analysis. This makes our approach flexible in selecting null markers. In our simulations, using a number of 30 or more null loci can effectively remove the bias and variance distortion. It is also shown that, even the null loci are weakly linked to the disease locus, the proposed method can also provide satisfactory correction.

作者 YUAN Min CUI WenQuan YANG YaNing

机构地区 School of Mathematics Department of Statistics and Finance

出处《Science China Mathematics》 SCIE 2012年第6期1127-1135,共9页 中国科学：数学（英文版）

基金 supported by National Natural Science Foundation of China(Grant No. 10971210) China Postdoctoral Science Foundation (Grant No. 20110490824)

关键词 affected sib-pairs bias null marker half sib-pairs variance distortion identical-by-descent （IBD）连锁分析不确定性偏见基因标记纠正受灾关联分析疾病基因

分类号 Q348 [生物学—遗传学] TP13 [自动化与计算机技术—控制理论与控制工程]

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Correcting for biases in affected sib-pair linkage analysis caused by uncertainty in sibling relationship

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