Integrating common and rare genetic variation in diverse human populations

Altshuler, David; Gibbs, Richard A.; Peltonen, Leena; Dermitzakis, Emmanouil T.; Schaffner, Stephen F.; Yu, Fuli; Bonnen, Penelope E.; Piw., de Bakker; Deloukas, Panos; Gabriel, Stacey; Gwilliam, Rhian; Hunt, Sarah; Inouye, Michael; Jia, Xiaoming; Palotie, Aarno; Parkin, Melissa; Whittaker, Pamela; Chang, Kyle; Hawes, Alicia; Lewis, Lora; Ren, Yanru; Wheeler, David A.; Muzny, Donna M.; Barnes, C.; Darvishi, Katayoon; Hurles, Matthew E.; Korn, Joshua M.; Kristiansson, Kati; Lee, C; McCarrol, S A; Nemesh, James; Keinan, Alon; Montgomery, Stephen B.; Pollack, Samuela; Price, Alkes L.; Soranzo, Nicole; Gonzaga‐Jauregui, Claudia; Anttila, Vesa; Brodeur, Wendy; Daly, Mark J.; Leslie, Stephen; McVean, Gil; Moutsianas, Loukas; Nguyen, Huy; Zhang, Q; Mjr., Ghori; McGinnis, Ralph; McLaren, William; Takeuchi, Fumihiko; Grossman,; Shlyakhter, Ilya; Hostetter, Elizabeth; Sabeti, Pardis C.; Adebamowo, Clement; Foster, Morris W.; Гордон,; Licinio, Júlio; Manca, Mario; Marshall, Patricia A.; Matsuda, Ichiro; Ngare, Duncan; Wang, V O; Reddy, D. Nageshwar; Rotimi, Charles N.; Royal, Charmaine; Sharp, Richard R.; Zeng, Changqing; Brooks, Lisa; McEwen, Jean

doi:10.1038/nature09298

Cited by 2,554 publications

(1,485 citation statements)

References 26 publications

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“…The development of genetic maps covering much of the genome led to linkage analyses in extended MS affected families from a number of countries, primarily of European ancestry 23, 24, 25, 26, 27, 28, 29, 30, 31, 32. These validated the HLA association but showed no significant linkage to loci outside the MHC.…”

Section: Early Genetic Studiesmentioning

confidence: 99%

“…The completion of the human genome sequencing project led to the development of complete catalogues of common genetic variation across the genome, and concomitant technologies to assay these variants in a cost‐effective and high‐throughput manner 25, 26. This technological development enabled the profiling of thousands of samples in a single study and prompted a shift away from family studies, where samples are necessarily limited and ascertainment challenging, to population‐based association studies comparing unrelated cases and controls 27.…”

Section: Genome‐wide Association Studiesmentioning

confidence: 99%

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Genome‐wide association studies of multiple sclerosis

Cotsapas¹,

Mitrovič

2018

Clin & Trans Imm

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Large‐scale genetic studies of multiple sclerosis have identified over 230 risk effects across the human genome, making it a prototypical common disease with complex genetic architecture. Here, after a brief historical background on the discovery and definition of the disease, we summarise the last fifteen years of genetic discoveries and map out the challenges that remain to translate these findings into an aetiological framework and actionable clinical understanding.

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Section: Early Genetic Studiesmentioning

confidence: 99%

Section: Genome‐wide Association Studiesmentioning

confidence: 99%

Genome‐wide association studies of multiple sclerosis

Cotsapas¹,

Mitrovič

2018

Clin & Trans Imm

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“…The HapMap project, which was started in 2003[89], has genotyped four million Single Nucleotide Polymorphisms (SNPs) in 1301 individuals from eleven populations distributed across the world[90]. The data has provided an abundance of information on common SNPs and their association with human disease, but many variants, including disease-causing variants, that occur at a low allele frequency in the population have been missed.…”

Section: Mps Applications In Mutation Analysismentioning

confidence: 99%

Direct mutation analysis by high-throughput sequencing: From germline to low-abundant, somatic variants

Gundry

Vijg

2012

Mutation Research/Fundamental and Molecular Mechanisms of Mutag

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DNA mutations are the source of genetic variation within populations. The majority of mutations with observable effects are deleterious. In humans mutations in the germ line can cause genetic disease. In somatic cells multiple rounds of mutations and selection lead to cancer. The study of genetic variation has progressed rapidly since the completion of the draft sequence of the human genome. Recent advances in sequencing technology, most importantly the introduction of massively parallel sequencing (MPS), have resulted in more than a hundred-fold reduction in the time and cost required for sequencing nucleic acids. These improvements have greatly expanded the use of sequencing as a practical tool for mutation analysis. While in the past the high cost of sequencing limited mutation analysis to selectable markers or small forward mutation targets assumed to be representative for the genome overall, current platforms allow whole genome sequencing for less than $5,000. This has already given rise to direct estimates of germline mutation rates in multiple organisms including humans by comparing whole genome sequences between parents and offspring. Here we present a brief history of the field of mutation research, with a focus on classical tools for the measurement of mutation rates. We then review MPS, how it is currently applied and the new insight into human and animal mutation frequencies and spectra that has been obtained from whole genome sequencing. While great progress has been made, we note that the single most important limitation of current MPS approaches for mutation analysis is the inability to address low-abundance mutations that turn somatic tissues into mosaics of cells. Such mutations are at the basis of intra-tumor heterogeneity, with important implications for clinical diagnosis, and could also contribute to somatic diseases other than cancer, including aging. Some possible approaches to gain access to low-abundance mutations are discussed, with a brief overview of new sequencing platforms that are currently waiting in the wings to advance this exploding field even further.

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“…Recent studies have made clear that relative to expectations for constantsized populations human sequence variation shows a strong excess of rare variants, most probably owing to population growth [64,65]. When designing mapping studies to discover novel resistance variants, we must keep these expectations in consideration.…”

Section: Synthesismentioning

confidence: 99%

Human population structure and the adaptive response to pathogen-induced selection pressures

Novembre

Han

2012

Phil. Trans. R. Soc. B

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The past few years of research in human evolutionary genetics have provided novel insights and questions regarding how human adaptations to recent selective pressures have taken place. Here, we review the advances most relevant to understanding human evolution in response to pathogen-induced selective pressures. Key insights come from theoretical models of adaptive evolution, particularly those that consider spatially structured populations, and from empirical population genomic studies of adaptive evolution in humans. We also review the CCR5-D32 HIV resistance allele as a case study of pathogen resistance in humans. Taken together, the results make clear that the human response to pathogen-induced selection pressures depends on a complex interplay between the age of the pathogen, the genetic basis of potential resistance phenotypes, and how population structure impacts the adaptive process in humans.

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Integrating common and rare genetic variation in diverse human populations

Cited by 2,554 publications

References 26 publications

Genome‐wide association studies of multiple sclerosis

Genome‐wide association studies of multiple sclerosis

Direct mutation analysis by high-throughput sequencing: From germline to low-abundant, somatic variants

Human population structure and the adaptive response to pathogen-induced selection pressures

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