Association between a common immunoglobulin heavy chain allele and rheumatic heart disease risk in Oceania

Parks, Tom; Mirabel, Mariana; Kado, Joseph; Auckland, Kathryn; Nowak, Jarosław; Rautanen, Anna; Mentzer, Alexander J.; Marijon, Éloi; Jouven, Xavier; Perman, Mai Ling; Cua, Tuliana; Kauwe, John; Allen, J. R. L.; Taylor, Henry M.; Robson, Kathryn; Deane, Charlotte M.; Steer, Andrew C.; Hill, Adrian V. S.

doi:10.1038/ncomms14946

Cited by 115 publications

(117 citation statements)

References 67 publications

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“…To date, few diseases have been robustly associated to IGH 22,23,70,71 . We previously suggested this was due to sparse locus coverage of genotyping arrays and an inability of array SNPs to tag functional IGH variants 4,20 .…”

Section: Discussionmentioning

confidence: 99%

“…We explored the potential advantage of our genotyping approach compared to array genotyping and imputation. We applied our long-read capture method to a sample selected from a recent rheumatic heart disease (RHD) GWAS 22 , which identified IGH as the primary risk locus. Direct genotyping in this sample was carried out previously using the HumanCore-24 BeadChip (n=14 SNVs) and targeted Sanger sequencing (n=8 SNVs); genotypes at additional SNVs were imputed with IMPUTE2 59 , using a combination of 1KGP and population-specific sequencing data as a reference set.…”

Section: Effects Of False-positive and -Negative Variants On Imputatimentioning

confidence: 99%

“…As a result, IGH has been largely overlooked by genome-wide studies, leaving our understanding of the contribution of IGH polymorphism to antibody-mediated immunity incomplete 4,20,21 . While early studies uncovered associations to disease susceptibility within IGH, few links have been made by genome-wide association studies (GWAS) and whole genome sequencing (WGS) 20,22,23 . Moreover, little is known about the genetic regulation of the human Ab response, despite evidence that features of the Ab repertoire are heritable 12,19,[24][25][26][27][28][29] To define the role of IGH variation in Ab function and disease, all classes of variation must be resolved 3,12,15,19,29,30 .…”

Section: Introductionmentioning

confidence: 99%

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A novel framework for characterizing genomic haplotype diversity in the human immunoglobulin heavy chain locus

Rodriguez

Gibson

Parks

et al. 2020

Preprint

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An incomplete ascertainment of genetic variation within the highly polymorphic immunoglobulin heavy chain locus (IGH) has hindered our ability to define genetic factors that influence antibody and B cell mediated processes. To date, methods for locus-wide genotyping of all IGH variant types do not exist. Here, we combine targeted long-read sequencing with a novel bioinformatics tool, IGenotyper, to fully characterize genetic variation within IGH in a haplotype-specific manner. We apply this approach to eight human samples, including a haploid cell line and two mother-father-child trios, and demonstrate the ability to generate high-quality assemblies (>98% complete and >99% accurate), genotypes, and gene annotations, including 2 novel structural variants and 17 novel gene alleles. We show that multiplexing allows for scaling of the approach without impacting data quality, and that our genotype call sets are more accurate than short-read (>35% increase in true positives and >97% decrease in false-positives) and array/imputation-based datasets. This framework establishes a foundation for leveraging IG genomic data to study population-level variation in the antibody response.

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Section: Discussionmentioning

confidence: 99%

Section: Effects Of False-positive and -Negative Variants On Imputatimentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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A novel framework for characterizing genomic haplotype diversity in the human immunoglobulin heavy chain locus

Rodriguez

Gibson

Parks

et al. 2020

Preprint

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“…Some allelic variants have been associated with increased disease susceptibility 27, 28 , yet the impact of immunoglobulin gene variation on disease risks is still unknown 29 . These regions have not been sufficiently covered in the numerous genome wide association studies performed to date.…”

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confidence: 99%

Polymorphisms in immunoglobulin heavy chain variable genes and their upstream regions

Mikocziova

Gidoni

Lindeman

et al. 2020

Preprint

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14Germline variations in immunoglobulin genes influence the repertoire of B cell receptors and 15 antibodies, and such polymorphisms may impact disease susceptibility. However, the knowledge of 16 the genomic variation of the immunoglobulin loci is scarce. Here, we report 25 novel germline IGHV 17 alleles as inferred from rearranged naïve B cell cDNA repertoires of 98 individuals. Thirteen novel 18 alleles were selected for validation, out of which ten were successfully confirmed by targeted 19 amplification and Sanger sequencing of non-B cell DNA. Moreover, we detected a high degree of 20 variability upstream of the V-region in the 5'UTR, leader 1, and leader 2 sequences, and found that These loci remain incompletely characterized due to the fact that they contain many repetitive 35 sequence segments with many duplicated genes 4 , which makes it difficult to correctly assemble short 36 reads from whole genome sequencing. Single nucleotide polymorphisms as well as copy number 37 variations are in linkage disequilibrium and make up distinct haplotypes 4 . To this date, a limited 38 number of genomically sequenced 5-7 and inferred 8,9 haplotypes of the heavy chain and the two light 39 chain loci have been described. Different databases exist for genomic immune receptor DNA 40 sequences (IMGT/GENE-DB 10 ), putative novel variants from inferred data (IgPdb 11 ) or entire immune 41 receptor repertoires (OGRDB 12 ). 42The usage of immunoglobulin heavy chain variable (IGHV) genes and their mutational status are most 43 frequently studied in relation to cancer 13,14 , responses to vaccines 15,16 , or in autoimmune diseases [17][18][19] . 44Most IGHV genes have several allelic variants and more alleles are being discovered as a result of 45 adaptive immune receptor repertoire-sequencing (AIRR-seq) 20,21 . Software tools such as TIgGER 22,23 , 46IgDiscover 24 and partis 25 allow to infer germline alleles from such repertoire data. Based on these 47 inferred alleles, the data can then be input to other tools that infer haplotypes and repertoire 48 deletions 26 . Incorrect annotation could possibly lead to inferring wrong deletions and biased 49 assessments. Therefore, having a full overview of germline variants is essential for studying the 50 adaptive immune response with high accuracy.51 Some allelic variants have been associated with increased disease susceptibility 27,28 , yet the impact of 52 immunoglobulin gene variation on disease risks is still unknown 29 . These regions have not been 53 sufficiently covered in the numerous genome wide association studies performed to date. More 54 comprehensive maps of polymorphisms are required for proper analysis. 55Here, we have used previously generated AIRR-seq data 30 from naïve B-cells of 98 Norwegian 56 individuals to identify novel IGHV alleles, a selection of which we then validated from genomic DNA 57 (gDNA) of non-B cells, i.e. T cells and monocytes. We also analyzed the sequences upstream of the 58 V-region, and constructed consensus sequences for the upstream variant...

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“…The top three applicants are invited to present their work at the Autumn Meeting, to compete for the Bernard and Joan Marshall Young Investigator Prize. In 2017, the three candidates selected to present were Dr Tom Parks from the University of Oxford who discussed his paper entitled ‘Association between a common immunoglobulin heavy chain allele and rheumatic heart disease risk in Oceania’1; Dr Eylem Levelt from the University of Leicester who presented her work on ‘Cardiac energetics, oxygenation, and perfusion during increased workload in patients with type two diabetes mellitus’2; and Dr Johannes Bargehr from the University of Cambridge (figure 1) who presented his data on ‘Human embryonic stem cell-derived epicardial cells augment cardiomyocyte-driven heart regeneration’ (under review). All three talks were stimulating and informative and resulted in lively question-and-answer sessions.…”

mentioning

confidence: 99%

Bernard and Joan Marshall Awards at the autumn meeting of the British Society for Cardiovascular Research 2017

Carr

Dodd

Heather

2018

Heart

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Association between a common immunoglobulin heavy chain allele and rheumatic heart disease risk in Oceania

Cited by 115 publications

References 67 publications

A novel framework for characterizing genomic haplotype diversity in the human immunoglobulin heavy chain locus

A novel framework for characterizing genomic haplotype diversity in the human immunoglobulin heavy chain locus

Polymorphisms in immunoglobulin heavy chain variable genes and their upstream regions

Bernard and Joan Marshall Awards at the autumn meeting of the British Society for Cardiovascular Research 2017

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