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XB-ART-51546
Proc Natl Acad Sci U S A 2012 Jul 24;10930:11920-7.
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A public resource facilitating clinical use of genomes.

Ball MP , Thakuria JV , Zaranek AW , Clegg T , Rosenbaum AM , Wu X , Angrist M , Bhak J , Bobe J , Callow MJ , Cano C , Chou MF , Chung WK , Douglas SM , Estep PW , Gore A , Hulick P , Labarga A , Lee JH , Lunshof JE , Kim BC , Kim JI , Li Z , Murray MF , Nilsen GB , Peters BA , Raman AM , Rienhoff HY , Robasky K , Wheeler MT , Vandewege W , Vorhaus DB , Yang JL , Yang L , Aach J , Ashley EA , Drmanac R , Kim SJ , Li JB , Peshkin L , Seidman CE , Seo JS , Zhang K , Rehm HL , Church GM .


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Rapid advances in DNA sequencing promise to enable new diagnostics and individualized therapies. Achieving personalized medicine, however, will require extensive research on highly reidentifiable, integrated datasets of genomic and health information. To assist with this, participants in the Personal Genome Project choose to forgo privacy via our institutional review board- approved "open consent" process. The contribution of public data and samples facilitates both scientific discovery and standardization of methods. We present our findings after enrollment of more than 1,800 participants, including whole-genome sequencing of 10 pilot participant genomes (the PGP-10). We introduce the Genome-Environment-Trait Evidence (GET-Evidence) system. This tool automatically processes genomes and prioritizes both published and novel variants for interpretation. In the process of reviewing the presumed healthy PGP-10 genomes, we find numerous literature references implying serious disease. Although it is sometimes impossible to rule out a late-onset effect, stringent evidence requirements can address the high rate of incidental findings. To that end we develop a peer production system for recording and organizing variant evaluations according to standard evidence guidelines, creating a public forum for reaching consensus on interpretation of clinically relevant variants. Genome analysis becomes a two-step process: using a prioritized list to record variant evaluations, then automatically sorting reviewed variants using these annotations. Genome data, health and trait information, participant samples, and variant interpretations are all shared in the public domain-we invite others to review our results using our participant samples and contribute to our interpretations. We offer our public resource and methods to further personalized medical research.

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References [+] :
Abecasis, A map of human genome variation from population-scale sequencing. 2010, Pubmed