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The Ashkenazi Genome Project. Shai Carmi Pe’er lab, Columbia University and The Ashkenazi Genome Consortium (TAGC). ASHG 2013, Boston. Why Study Ashkenazi Jewish Genetics?. Unique demography conducive to medical genetics A severe founder event; isolation Large current size
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The Ashkenazi Genome Project Shai Carmi Pe’er lab, Columbia University and The Ashkenazi Genome Consortium (TAGC) ASHG 2013, Boston
Why Study Ashkenazi Jewish Genetics? • Unique demography conducive to medical genetics • A severe founder event; isolation • Large current size • Many genetic risk factors discovered • Sequencing panel missing Palamara et al., 2012
Why Study Ashkenazi Jewish Genetics? • Unique demography conducive to medical genetics • Population genetics • Insight on both European and Middle-Eastern past AJ Europeans Jewish, non-AJ Price et al., 2008 Olshen et al., 2008 Need et al., 2009 Kopelman et al., 2009Behar et al., 2010 Bray et al., 2010 Guha et al., 2012 Middle-Eastern Atzmon et al., 2010
The Ashkenazi Genome Consortium NY area labs interested in specific diseases Study design: • 128 unrelated healthy controls • PCA-validated AJ ancestry • High-coverage whole-genome sequencing • Complete Genomics Learn about population history Quantify utility in medical genetics
Variant Discovery & Screening • Comparison cohort: 26 Flemish individuals from Belgium • AJ have more novel variants than FL • Variant discovery in AJ predicted to decay faster Method: Gravel et al., 2011
Variant Discovery & Screening • Comparison cohort: 26 Flemish individuals from Belgium • Most novel AJ variants do not appear in a FL panel
Variant Discovery & Screening • Comparison cohort: 26 Flemish individuals from Belgium • Most novel AJ variants do not appear in a FL panel • Many novel AJ variants appear in an AJ panel
Variant Discovery & Screening • Comparison cohort: 26 Flemish individuals from Belgium • Most novel AJ variants do not appear in a FL panel • Many novel AJ variants appear in an AJ panel
Abundance of Genetic Sharing • Sharing common in AJ (but not in FL or between AJ-FL) • Long segments shared with the panel cover the majority of a typical AJ genome >3cM Theory predicts the average coverage:
Recent AJ History Method: Palamara et al., 2012
The Joint Allele Frequency Spectrum • Allele frequencies correlated, but populations distinct • Fit a historical model to the AFS.
Time (years ago) A Model Present AJ FL
Time (years ago) The Inferred Model 6500 Out-of-Africa 52k 2300 Middle-East 1800 Early Neolithic migrants 10.8k Jewish diaspora 1.7k 55% Present AJ FL Method: Gutenkunstet al., 2009
Summary • Data: 128 high coverage AJ genomes • Medical genetics:Useful for genome screening and imputation • Population genetics: • Recent severe bottleneck and rapid expansion • Over 50% European ancestry in AJ • Europeans diverged from ME only ≈10-20 kya
Thank you! TAGC consortium members: Columbia University Computer Science: Itsik Pe’erFillan Grady, Ethan Kochav, James XueShlomo Hershkop Long-Island Jewish Medical Center: Todd Lencz, Semanti Mukherjee, SauravGuha Columbia University Medical Center: Lorraine Clark, Xinmin Liu Albert Einstein College of Medicine: Gil Atzmon, Harry Ostrer, NirBarzilai, KinnariUpadhyay, Danny Ben-Avraham Mount Sinai School of Medicine: Inga Peter, Laurie Ozelius Memorial Sloan Kettering Cancer Center: Ken Offit, Joseph Vijai Yale School of Medicine: Judy Cho, Ken Hui, Monica Bowen The Hebrew University of Jerusalem: Ariel Darvasi Beth Israel Medical Center: Susan Bressman VIB, Gent, Belgium Herwig Van Marck, StephanePlaisance Complete GenomicsOmicia Funding: Human Frontiers Science program