The immunoglobulin heavy chain locus: genetic variation, missing data, and implications for human disease

Watson, Corey T.; Breden, Felix

doi:10.1038/gene.2012.12

Cited by 167 publications

(192 citation statements)

References 84 publications

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“…Subjects also differ greatly in the set of V(D)J segment alleles that they carry (6,19,21) and some V segment alleles have been associated with disease (including SLE, MS, RA, and type 1 diabetes, as summarized in ref. 5). Along with the underlying genetics of the Ig locus, properties of the expressed B-cell Ig repertoire, such as diversity, have been associated with disease and clinical status (5-10).…”

Section: Discussionmentioning

confidence: 99%

“…Although IGHV genes can be duplicated in some subjects, with IGHV1-69 being a frequent example (as reviewed in ref. 5), it is expected that each subject carries either one or two alleles of most genes. However, IMGT/HighV-QUEST assigned an average of 4.3 alleles per gene across the three subjects sequenced by 454, as shown in Table 1.…”

Section: Automated Methods Detects Novel Ighv Alleles From Experimentalmentioning

confidence: 99%

“…Previous studies have, for example: revealed the association of certain germline genotypes with susceptibility to such diseases as rheumatoid arthritis (RA), systemic lupus erythematosus (SLE), and multiple sclerosis (MS) (5,6); found correlations of age with a reduced Ig clonal diversity and less intense response to immune challenge (7,8); found overly expanded clones in cases of lymphoma (9,10); and discovered convergent Ig evolution across subjects in response to certain immune challenges (11,12). These repertoire-sequencing (Rep-Seq) studies have benefitted from improvements in sequencing technologies, which allow for the generation of millions of reads per run (13).…”

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confidence: 99%

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Automated analysis of high-throughput B-cell sequencing data reveals a high frequency of novel immunoglobulin V gene segment alleles

Gadala-Maria

Yaari

Uduman³

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

199

235

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Individual variation in germline and expressed B-cell immunoglobulin (Ig) repertoires has been associated with aging, disease susceptibility, and differential response to infection and vaccination. Repertoire properties can now be studied at large-scale through next-generation sequencing of rearranged Ig genes. Accurate analysis of these repertoire-sequencing (Rep-Seq) data requires identifying the germline variable (V), diversity (D), and joining (J) gene segments used by each Ig sequence. Current V(D)J assignment methods work by aligning sequences to a database of known germline V(D)J segment alleles. However, existing databases are likely to be incomplete and novel polymorphisms are hard to differentiate from the frequent occurrence of somatic hypermutations in Ig sequences. Here we develop a Tool for Ig Genotype Elucidation via Rep-Seq (TIgGER). TIgGER analyzes mutation patterns in Rep-Seq data to identify novel V segment alleles, and also constructs a personalized germline database containing the specific set of alleles carried by a subject. This information is then used to improve the initial V segment assignments from existing tools, like IMGT/HighV-QUEST. The application of TIgGER to Rep-Seq data from seven subjects identified 11 novel V segment alleles, including at least one in every subject examined. These novel alleles constituted 13% of the total number of unique alleles in these subjects, and impacted 3% of V(D)J segment assignments. These results reinforce the highly polymorphic nature of human Ig V genes, and suggest that many novel alleles remain to be discovered. The integration of TIgGER into Rep-Seq processing pipelines will increase the accuracy of V segment assignments, thus improving B-cell repertoire analyses.next-generation sequencing | B-cell repertoire | adaptive immunity | somatic hypermutation | variable gene segment T he production by B cells of immunoglobulin (Ig) proteins, which are expressed on the cell surface as B-cell receptors and secreted by subsets of B cells as antibodies, is a key component of the adaptive immune system in humans. Through their specific binding to an enormously diverse range of foreign bodies, Ig proteins are able to elicit further immunological response and provide protection. These proteins are assembled in B cells from two pairs of polypeptide chains, termed heavy and light. The antigen-binding portions of these genes are created through the somatic recombination of gene segments, termed variable (V), diversity (D), and joining (J). During the recombination process, one each of the ∼46 V, 23 D, and 6 J gene segments (1) recombine to make the antigen-binding region of the heavy chain; the light chain is created by a similar process, although involving one of two different loci (λ and κ) containing V and J genes only. Over three million different Ig sequences can be created through this V(D)J recombinatorial process alone (2). The potential diversity of these sequences is further expanded to the order of trillions (2) when combined with the random insert...

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Section: Discussionmentioning

confidence: 99%

Section: Automated Methods Detects Novel Ighv Alleles From Experimentalmentioning

confidence: 99%

mentioning

confidence: 99%

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Automated analysis of high-throughput B-cell sequencing data reveals a high frequency of novel immunoglobulin V gene segment alleles

Gadala-Maria

Yaari

Uduman³

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

199

235

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“…Homozygous deletions of IGHV3‐30*01 and IGHV3‐30‐3 were found to be enriched 2·8‐fold in SLE patients with nephritis compared with ethnically matched healthy individuals, and SLE patients with these deletions exhibited higher titres of anti‐DNA antibodies 30, 31. This deletion has also been shown to be associated with susceptibility to chronic idiopathic thrombocytopaenic purpura32 and Kawasaki disease33 (reviewed in Watson et al 34…”

Section: Slementioning

confidence: 99%

Antibody repertoire analysis in polygenic autoimmune diseases

2018

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SummaryHigh‐throughput sequencing of the DNA/RNA encoding antibody heavy‐ and light‐chains is rapidly transforming the field of adaptive immunity. It can address key questions, including: (i) how the B‐cell repertoire differs in health and disease; and (ii) if it does differ, the point(s) in B‐cell development at which this occurs. The advent of technologies, such as whole‐genome sequencing, offers the chance to link abnormalities in the B‐cell antibody repertoire to specific genomic variants and polymorphisms. Here, we discuss the current research using B‐cell antibody repertoire sequencing in three polygenic autoimmune diseases where there is good evidence for a pathological role for B‐cells, namely systemic lupus erythematosus, multiple sclerosis and rheumatoid arthritis. These autoimmune diseases exhibit significantly skewed B‐cell receptor repertoires compared with healthy controls. Interestingly, some common repertoire defects are shared between diseases, such as elevated IGHV4‐34 gene usage. B‐cell clones have effectively been characterized and tracked between different tissues and blood in autoimmune disease. It has been hypothesized that these differences may signify differences in B‐cell tolerance; however, the mechanisms and implications of these defects are not clear.

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“…Each H chain gene is formed somatically and stochastically by recombination and joining of one each of the ∼55 immunoglobulin heavy chain variable (IGHV), ∼27 immunoglobulin heavy chain diversity (IGHD), and 6 immunoglobulin heavy chain joining (IGHJ) genes. Each L chain gene is similarly formed by using one of either ∼40 immunoglobulin kappa variable (IGKV) or ∼30 immunoglobulin lambda variable (IGLV) genes, recombined with one of either 5 immunoglobulin kappa joining (IGKJ) or 4 immunoglobulin lambda joining (IGLJ) genes (4). There is evidence that certain V genes are more frequently used in autoantibodies, such as IGHV1-69 (5), and certain families of V genes are overexpressed in particular diseases, e.g., Graves disease (IGHV1 family), Hashimoto disease (IGHV3 family), myasthenia gravis, chronic idiopathic thrombocytopenic purpura (IGHV3-30), and Sjogren disease (IGHV1-69 and IGHV3-7) (6).…”

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confidence: 99%

Characterization of pathogenic human monoclonal autoantibodies against GM-CSF

Wang

Thomson

Allan

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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The origin of pathogenic autoantibodies remains unknown. Idiopathic pulmonary alveolar proteinosis is caused by autoantibodies against granulocyte–macrophage colony-stimulating factor (GM-CSF). We generated 19 monoclonal autoantibodies against GM-CSF from six patients with idiopathic pulmonary alveolar proteinosis. The autoantibodies used multiple V genes, excluding preferred V-gene use as an etiology, and targeted at least four nonoverlapping epitopes on GM-CSF, suggesting that GM-CSF is driving the autoantibodies and not a B-cell epitope on a pathogen cross-reacting with GM-CSF. The number of somatic mutations in the autoantibodies suggests that the memory B cells have been helped by T cells and re-entered germinal centers. All autoantibodies neutralized GM-CSF bioactivity, with general correlations to affinity and off-rate. The binding of certain autoantibodies was changed by point mutations in GM-CSF that reduced binding to the GM-CSF receptor. Those monoclonal autoantibodies that potently neutralize GM-CSF may be useful in treating inflammatory disease, such as rheumatoid arthritis and multiple sclerosis, cancer, and pain.

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The immunoglobulin heavy chain locus: genetic variation, missing data, and implications for human disease

Cited by 167 publications

References 84 publications

Automated analysis of high-throughput B-cell sequencing data reveals a high frequency of novel immunoglobulin V gene segment alleles

Automated analysis of high-throughput B-cell sequencing data reveals a high frequency of novel immunoglobulin V gene segment alleles

Antibody repertoire analysis in polygenic autoimmune diseases

Characterization of pathogenic human monoclonal autoantibodies against GM-CSF

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