Paired-end mapping reveals extensive structural variation in the human genome |
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| Authors: | Korbel Jan O Urban Alexander Eckehart Affourtit Jason P Godwin Brian Grubert Fabian Simons Jan Fredrik Kim Philip M Palejev Dean Carriero Nicholas J Du Lei Taillon Bruce E Chen Zhoutao Tanzer Andrea Saunders A C Eugenia Chi Jianxiang Yang Fengtang Carter Nigel P Hurles Matthew E Weissman Sherman M Harkins Timothy T Gerstein Mark B Egholm Michael Snyder Michael |
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| Institution: | Molecular Biophysics and Biochemistry Department, Yale University, New Haven, CT 06520, USA. |
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| Abstract: | Structural variation of the genome involves kilobase- to megabase-sized deletions, duplications, insertions, inversions, and complex combinations of rearrangements. We introduce high-throughput and massive paired-end mapping (PEM), a large-scale genome-sequencing method to identify structural variants (SVs) approximately 3 kilobases (kb) or larger that combines the rescue and capture of paired ends of 3-kb fragments, massive 454 sequencing, and a computational approach to map DNA reads onto a reference genome. PEM was used to map SVs in an African and in a putatively European individual and identified shared and divergent SVs relative to the reference genome. Overall, we fine-mapped more than 1000 SVs and documented that the number of SVs among humans is much larger than initially hypothesized; many of the SVs potentially affect gene function. The breakpoint junction sequences of more than 200 SVs were determined with a novel pooling strategy and computational analysis. Our analysis provided insights into the mechanisms of SV formation in humans. |
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