Genome-wide in situ exon capture for selective resequencing

被引:453
作者
Hodges, Emily
Xuan, Zhenyu
Balija, Vivekanand
Kramer, Melissa
Molla, Michael N.
Smith, Steven W.
Middle, Christina M.
Rodesch, Matthew J.
Albert, Thomas J.
Hannon, Gregory J.
McCombie, W. Richard
机构
[1] Cold Spring Harbor Lab, Warson Sch Biol Sci, Cold Spring Harbor, NY 11724 USA
[2] Howard Hughes Med Inst, Watson Sch Biol Sci, Cold Spring Harbor, NY USA
[3] NimbleGlen Syst Inc, Madison, WI 53711 USA
基金
美国国家科学基金会; 美国国家卫生研究院;
关键词
D O I
10.1038/ng.2007.42
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Increasingly powerful sequencing technologies are ushering in an era of personal genome sequences and raising the possibility of using such information to guide medical decisions. Genome resequencing also promises to accelerate the identification of disease-associated mutations. Roughly 98% of the human genome is composed of repeats and intergenic or non-proteincoding sequences. Thus, it is crucial to focus resequencing on high-value genomic regions. Protein-coding exons represent one such type of high-value target. We have developed a method of using flexible, high-density microarrays to capture any desired fraction of the human genome, in this case corresponding to more than 200,000 protein-coding exons. Depending on the precise protocol, up to 55-85% of the captured fragments are associated with targeted regions and up to 98% of intended exons can be recovered. This methodology provides an adaptable route toward rapid and efficient resequencing of any sizeable, non-repeat portion of the human genome.
引用
收藏
页码:1522 / 1527
页数:6
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