A high-resolution recombination map of the human genome

Kong, Augustine; Guðbjartsson, Daníel F.; Sainz, Jesús; Jónsdóttir, Guðrún; Gudjonsson, Sigurjon A.; Richardsson, Bjorgvin; Sigurðardóttir, Sigrún; Barnard, John; Hallbeck, Björn; Másson, Gísli; Shlien, Adam; Palsson, Stefan; Frigge, Michael L.; Thorgeirsson, Thorgeir E.; Gulcher, Jeffrey R.; Stefánsson, Kāri

doi:10.1038/ng917

Cited by 1,557 publications

(1,728 citation statements)

References 23 publications

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“…40 This points to high LD over the region, which has already been reported by Ueda et al 7 Our results not only show this high LD but also that it persists across populations worldwide. Previous studies in other genes, such as PAH 41 or the PKLR-GBA gene region, 42 have shown a general pattern of moderate geographical structure of LD with higher values out of Africa and low values in sub-Saharan Africa.…”

Section: Ld Patternssupporting

confidence: 82%

Haplotype tagging efficiency in worldwide populations in CTLA4 gene

et al. 2005

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The cytotoxic T lymphocyte antigen 4 (CTLA4) acts as a potent negative regulator of T-cell response, and has been suggested as a pivotal candidate gene for autoimmune disorders such as Graves' disease, type 1 diabetes and autoimmune hypothyroidism, among others. Several single-nucleotide polymorphisms (SNPs) have been proposed as the susceptibility variants, or to be in strong linkage disequilibrium (LD) with the variant. Nevertheless, contradictory results have been found, which may be due to lack of knowledge of the genetic structure of CTLA4 and its geographic variation. We have typed 17 SNPs throughout the CTLA4 gene region in order to analyze the haplotype diversity and LD structure in a worldwide population set (1262 individuals from 44 populations) to understand the variation pattern of the region. Allele and haplotype frequency differentiation between populations is consistent with genomewide averages and points to a lack of strong population-specific selection pressures. LD is high and its pattern is not significantly different within or between continents. However, haplotype composition is significantly different between geographical groups. A continent-specific set of haplotype tagging SNPs has been designed to be used for future association studies. These are portable among populations, although their efficiency might vary depending on the population haplotype spectrum.

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Section: Ld Patternssupporting

confidence: 82%

Haplotype tagging efficiency in worldwide populations in CTLA4 gene

et al. 2005

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“…We thus computed IBD for 342 'derivative' pedigrees (including 251 intact pedigrees, 51 reduced pedigree, and 40 newly derived pedigrees) for chromosome X multipoint analysis. For the autosomal markers, map distances were obtained from the Center for Medical Genetics (http://research.marshfieldclinic.org/genetics/) whenever available or estimated otherwise; map distances for the X chromosomes were obtained from DeCODE [40]. Marker allele frequencies were estimated from the genotypes of the study participants by simple allele counting; this method yielded allele frequency estimates very similar to those obtained by maximum likelihood estimation.…”

Section: Methodsmentioning

confidence: 99%

Proximal hip geometry is linked to several chromosomal regions: Genome-wide linkage results from the Framingham Osteoporosis Study

Demissie

Dupuis

Cupples

et al. 2007

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“…In general, we used the Marshfield map (http:// research.marshfieldclinic.org/genetics) with two exceptions: (1) If there was considerable disagreement between the Marshfield and deCODE maps, 54 we used our data set to resolve the marker order and distances; (2) If there was a large disagreement between the Marshfield map and our data set that could not be resolved, we used the distances provided in the deCODE map if possible, or if not we used our data set to estimate distances. On chromosome 2, the distance between D2S1326 and D2S2241 was almost twice as large, and the distances between markers D2S2241, D2S142 and D2S1353 were considerably smaller, in the deCODE map than in the Marshfield map.…”

Section: Genotypesmentioning

confidence: 99%

A genome scan in multigenerational families with dyslexia: Identification of a novel locus on chromosome 2q that contributes to phonological decoding efficiency

et al. 2005

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Dyslexia is a common and complex developmental disorder manifested by unexpected difficulty in learning to read. Multiple different measures are used for diagnosis, and may reflect different biological pathways related to the disorder. Impaired phonological decoding (translation of written words without meaning cues into spoken words) is thought to be a core deficit. We present a genome scan of two continuous measures of phonological decoding ability: phonemic decoding efficiency (PDE) and word attack (WA). PDE measures both accuracy and speed of phonological decoding, whereas WA measures accuracy alone. Multipoint variance component linkage analyses (VC) and Markov chain Monte-Carlo (MCMC) multipoint joint linkage and segregation analyses were performed on 108 families. A strong signal was observed on chromosome 2 for PDE using both VC (LOD ¼ 2.65) and MCMC methods (intensity ratio (IR) ¼ 32.1). The IR is an estimate of the ratio of the posterior to prior probability of linkage in MCMC analysis. The chromosome 2 signal was not seen for WA. More detailed mapping with additional markers provided statistically significant evidence for linkage of PDE to chromosome 2, with VC-LOD ¼ 3.0 and IR ¼ 59.6 at D2S1399. Parametric analyses of PDE, using a model obtained by complex segregation analysis, provided a multipoint maximum LOD ¼ 2.89. The consistency of results from three analytic approaches provides strong evidence for a locus on chromosome 2 that influences speed but not accuracy of phonological decoding. Molecular Psychiatry (2005) 10, 699-711.

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A high-resolution recombination map of the human genome

Cited by 1,557 publications

References 23 publications

Haplotype tagging efficiency in worldwide populations in CTLA4 gene

Haplotype tagging efficiency in worldwide populations in CTLA4 gene

Proximal hip geometry is linked to several chromosomal regions: Genome-wide linkage results from the Framingham Osteoporosis Study

A genome scan in multigenerational families with dyslexia: Identification of a novel locus on chromosome 2q that contributes to phonological decoding efficiency

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