Global diversity, population stratification, and selection of human copy-number variation

Sudmant, Peter H.; Mallick, Swapan; Nelson, Bradley J.; Hormozdiari, Fereydoun; Krumm, Niklas; Huddleston, John; Coe, Bradley P.; Baker, Carl; Nordenfelt, Susanne; Bamshad, Michael J.; Jorde, Lynn B.; Posukh, Olga L.; Sahakyan, Hovhannes; Watkins, W. Scott; Yepiskoposyan, Levon; Abdullah, Muhammad; Bravi, Cláudio M.; Capelli, Cristian; Hervig, Tor; Wee, Joseph; Tyler‐Smith, Chris; Driem, George van; Romero, Irene Gallego; Jha, Aashish R.; Karachanak-Yankova, Sena; Toncheva, Draga; Comas, David; Henn, Brenna M.; Kivisild, Toomas; Ruiz-Linares, Andrés; Sajantila, Antti; Metspalu, Ene; Parik, Jueri; Villems, Richard; Starikovskaya, Elena B.; Ayodo, George; Beall, Cynthia M.; Rienzo, Anna Di; Hammer, Michael F.; Хусаинова, Р. И.; Хуснутдинова, Э. К.; Klitz, William; Winkler, Cheryl A.; Labuda, Damian; Metspalu, Mait; Tishkoff, Sarah A.; Dryomov, Stanislav; Sukernik, Rem I.; Patterson, Nick; Reich, David; Eichler, Evan E.

doi:10.1126/science.aab3761

Cited by 302 publications

(338 citation statements)

References 57 publications

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“…Comparing our nonplatinum SNVs with a set of common, population-level CNVs (Sudmant et al 2015a) and CNV calls from this pedigree (Roller et al 2016) shows a significant excess of Category 1 and Category 4 SNVs overlapping duplications and significantly more Category 2 SNVs overlapping deletions (Supplemental Table S13). Overall, we conclude that the majority (∼75%) of nonplatinum SNVs in this analysis colocate with an unidentified germline or somatic variant; 67.3% were accounted for in 23,442 clusters (indicative of CNVs).…”

Section: 4m Variants Validated By Genetic Inheritancementioning

confidence: 99%

A reference data set of 5.4 million phased human variants validated by genetic inheritance from sequencing a three-generation 17-member pedigree

et al. 2016

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Improvement of variant calling in next-generation sequence data requires a comprehensive, genome-wide catalog of highconfidence variants called in a set of genomes for use as a benchmark. We generated deep, whole-genome sequence data of 17 individuals in a three-generation pedigree and called variants in each genome using a range of currently available algorithms. We used haplotype transmission information to create a phased "Platinum" variant catalog of 4.7 million singlenucleotide variants (SNVs) plus 0.7 million small (1-50 bp) insertions and deletions (indels) that are consistent with the pattern of inheritance in the parents and 11 children of this pedigree. Platinum genotypes are highly concordant with the current catalog of the National Institute of Standards and Technology for both SNVs (>99.99%) and indels (99.92%) and add a validated truth catalog that has 26% more SNVs and 45% more indels. Analysis of 334,652 SNVs that were consistent between informatics pipelines yet inconsistent with haplotype transmission ("nonplatinum") revealed that the majority of these variants are de novo and cell-line mutations or reside within previously unidentified duplications and deletions. The reference materials from this study are a resource for objective assessment of the accuracy of variant calls throughout genomes.

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Section: 4m Variants Validated By Genetic Inheritancementioning

confidence: 99%

A reference data set of 5.4 million phased human variants validated by genetic inheritance from sequencing a three-generation 17-member pedigree

et al. 2016

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“…We merged the South Asian and Ashkenazi Jewish data generated by the other Illumina arrays to create an "Illumina" dataset consisting of 172 individuals genotyped on 500,640 SNPs. We merged the data from the Affymetrix Human Origins arrays with the Ashkenazi Jewish data and data from the Simons Genome Diversity Project 19,20 to create a dataset with 4,402 individuals genotyped on 512,615 SNPs. We analyzed the four datasets separately due to the small intersection of SNPs between them.…”

Section: Data Setsmentioning

confidence: 99%

The promise of discovering population-specific disease-associated genes in South Asia

et al. 2017

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“…We find that the inverted H2 haplotype contains multiple, highly identical SDs in direct orientation that flank the disease-associated critical region (Supplemental Table 5; Supplemental Section 5.1); the largest of which, SD19 (∼385 kbp of >98% sequence identity), corresponds to the beta-defensin gene family cluster. We assessed the extent of normal copy number variation of this duplicated segment by measuring the aggregate beta-defensin copy number in 236 high-coverage human and 56 great ape genomes sequenced as part of the HGDP (Sudmant et al 2015a) and the Great Ape Genome Project (Prado-Martinez et al 2013). All great apes were diploid for this segment with the exception of human, chimpanzee, and bonobo.…”

Section: Copy Number Variationmentioning

confidence: 99%

“…We used SNV/indel calls from the Human Genome Diversity Project or HGDP (Sudmant et al 2015a) and the Phase III 1000 Genomes Project (Sudmant et al 2015b) mapped to GRCh37. HGDP genomes were phased using BEAGLE 4.0 (r1399).…”

Section: Population Genetic Analysismentioning

confidence: 99%

Interchromosomal core duplicons drive both evolutionary instability and disease susceptibility of the Chromosome 8p23.1 region

et al. 2016

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Recurrent rearrangements of Chromosome 8p23.1 are associated with congenital heart defects and developmental delay. The complexity of this region has led to inconsistencies in the current reference assembly, confounding studies of genetic variation. Using comparative sequence-based approaches, we generated a high-quality 6.3-Mbp alternate reference assembly of an inverted Chromosome 8p23.1 haplotype. Comparison with nonhuman primates reveals a 746-kbp duplicative transposition and two separate inversion events that arose in the last million years of human evolution. The breakpoints associated with these rearrangements map to an ape-specific interchromosomal core duplicon that clusters at sites of evolutionary inversion (P = 7.8 × 10(-5)). Refinement of microdeletion breakpoints identifies a subgroup of patients that map to the same interchromosomal core involved in the evolutionary formation of the duplication blocks. Our results define a higher-order genomic instability element that has shaped the structure of specific chromosomes during primate evolution contributing to rearrangements associated with inversion and disease

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Global diversity, population stratification, and selection of human copy-number variation

Cited by 302 publications

References 57 publications

A reference data set of 5.4 million phased human variants validated by genetic inheritance from sequencing a three-generation 17-member pedigree

A reference data set of 5.4 million phased human variants validated by genetic inheritance from sequencing a three-generation 17-member pedigree

The promise of discovering population-specific disease-associated genes in South Asia

Interchromosomal core duplicons drive both evolutionary instability and disease susceptibility of the Chromosome 8p23.1 region

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