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利用重组近交异质群体和体外异质群体进行数量性状基因座精细定位。

QTL fine-mapping with recombinant-inbred heterogeneous stocks and in vitro heterogeneous stocks.

作者信息

Valdar William S J, Flint Jonathan, Mott Richard

机构信息

Wellcome Trust Centre for Human Genetics, Roosevelt Drive, Oxford OX4 7AD, UK.

出版信息

Mamm Genome. 2003 Dec;14(12):830-8. doi: 10.1007/s00335-003-3021-1.

Abstract

We compared strategies to fine-map Quantitative Trait Loci (QTL) in mice with heterogeneous stocks (HS). We showed that a panel of about 100 Recombinant Inbred Lines (RIL) derived from an HS, and which we called an RIHS, was ideally suited to fine-map QTL to very high resolution, without the cost of additional genotyping. We also investigated a strategy based on in vitro fertilization of large numbers of F(1) offspring of HS males crossed with an inbred line (IVHS). This method required some additional genotyping but avoided the breeding delays and costs associated with the construction of an RI panel. We showed that QTL detection was higher by using RIHS than with IVHS and that it was independent of the number of RI lines, provided the total number of animals phenotyped was constant. However, fine-mapping accuracy was slightly better with IVHS. We also investigated the effects of varying the number of HS generations and using multiallelic microsatellites instead of SNPs. We found that quite modest generation times of 10-20 generations were optimal. Microsatellites were superior to SNPs only when the generation time was 30 or more and when the markers were widely spaced.

摘要

我们比较了在具有异质群体(HS)的小鼠中精细定位数量性状基因座(QTL)的策略。我们表明,一组约100个源自HS的重组近交系(RIL),我们称之为RIHS,非常适合将QTL精细定位到非常高的分辨率,而无需额外的基因分型成本。我们还研究了一种基于体外受精的策略,该策略涉及HS雄性与近交系杂交产生的大量F(1)后代(IVHS)。这种方法需要一些额外的基因分型,但避免了与构建RI群体相关的繁殖延迟和成本。我们表明,使用RIHS进行QTL检测比使用IVHS更高,并且只要表型分析的动物总数恒定,它就与RI系的数量无关。然而,IVHS的精细定位准确性略好。我们还研究了改变HS世代数量以及使用多等位基因微卫星而非单核苷酸多态性(SNP)的影响。我们发现10 - 20代这样相当适度的世代时间是最佳的。仅当世代时间为30代或更多且标记间隔很宽时,微卫星才优于SNP。

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