Polygenic burdens on cell-specific pathways underlie the risk of rheumatoid arthritis

Ishigaki, Kazuyoshi; Kochi, Yuta; Suzuki, Akari; Tsuchida, Yoshiaki; Tsuchiya, Haruka; Sumitomo, Shuji; Yamaguchi, Kensuke; Nagafuchi, Yasuo; Nakachi, Shinichiro; Kato, Rika; Sakurai, Keiichi; Shoda, Hirofumi; Ikari, Katsunori; Taniguchi, Atsuo; Yamanaka, Hisashi; Miya, Fuyuki; Tsunoda, Tatsuhiko; Okada, Yukinori; Momozawa, Yukihide; Kamatani, Yoichiro; Yamada, Ryo; Kubo, Michiaki; Fujio, Keishi; Yamamoto, Kazuhiko

doi:10.1038/ng.3885

Cited by 127 publications

(123 citation statements)

References 39 publications

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“…In a recent article in Arthritis & Rheumatology , Thalayasingam et al reported that the 6p23 locus, associated with rheumatoid arthritis (RA), has a B cell–specific expression quantitative trait locus (eQTL) effect on CD83. The B cell–specific eQTL effect at this locus is robust and has also been reported by others , and it presumably contributes to the pathogenesis of RA by decreasing the expression of CD83 on B cells. We sought to determine the basis for the B cell–specific eQTL effect and to further elucidate the mechanism by which it contributes to RA pathogenesis.…”

supporting

confidence: 77%

“…CD83 regulates the development of murine B cells . We therefore hypothesized that CD83 expression might influence the development of human B cells, and we examined the relationship between this haplotype and peripheral blood B cells in healthy subjects from our data set . Individuals with the RA risk SNP had an increased frequency of CD27−IgD− double‐negative B cells (Figure B), a subset that is increased in the peripheral blood of RA patients and thought to be pathogenic .…”

mentioning

confidence: 99%

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Reduction of CD83 Expression on B Cells and the Genetic Basis for Rheumatoid Arthritis: Comment on the Article by Thalayasingam et al

Tsuchida

Sumitomo

et al. 2018

Arthritis & Rheumatology

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supporting

confidence: 77%

mentioning

confidence: 99%

Reduction of CD83 Expression on B Cells and the Genetic Basis for Rheumatoid Arthritis: Comment on the Article by Thalayasingam et al

Tsuchida

Sumitomo

et al. 2018

Arthritis & Rheumatology

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“…In addition to the above‐mentioned analyses, ChIP‐Atlas Enrichment Analysis (formerly designated “ in silico ChIP”) has been used for various other purposes. For example, this tool has been applied to analyze TR enrichment at genomic ROIs such as expression quantitative trait loci (eQTLs), a user's own ChIP‐seq peak‐call data, and evolutionarily accelerated regions as well as genes whose expression levels are changed by drug exposure, aging, or cancer development (see http://chip-atlas.org/publications for the full list of publications citing ChIP‐Atlas). The results generated by ChIP‐Atlas are all assigned unique URLs (see ChIP‐Atlas document in https://github.com/inutano/chip-atlas/wiki for details) and are publicly available, and they are thus ready for sharing seamlessly among researchers for subsequent analysis in command lines and for interconnecting with other biodatabases such as the DeepBlue Epigenomic Data Server and RegulatorTrail , where ChIP‐Atlas data have been imported and subjected to analyses.…”

Section: Resultsmentioning

confidence: 99%

Ch IP ‐Atlas: a data‐mining suite powered by full integration of public Ch IP ‐seq data

Oki

Ohta

Shioi³

et al. 2018

EMBO Reports

626

469

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We have fully integrated public chromatin chromatin immunoprecipitation sequencing (ChIP‐seq) and DNase‐seq data (n > 70,000) derived from six representative model organisms (human, mouse, rat, fruit fly, nematode, and budding yeast), and have devised a data‐mining platform—designated ChIP‐Atlas (http://chip-atlas.org). ChIP‐Atlas is able to show alignment and peak‐call results for all public ChIP‐seq and DNase‐seq data archived in the NCBI Sequence Read Archive (SRA), which encompasses data derived from GEO, ArrayExpress, DDBJ, ENCODE, Roadmap Epigenomics, and the scientific literature. All peak‐call data are integrated to visualize multiple histone modifications and binding sites of transcriptional regulators (TRs) at given genomic loci. The integrated data can be further analyzed to show TR–gene and TR–TR interactions, as well as to examine enrichment of protein binding for given multiple genomic coordinates or gene names. ChIP‐Atlas is superior to other platforms in terms of data number and functionality for data mining across thousands of ChIP‐seq experiments, and it provides insight into gene regulatory networks and epigenetic mechanisms.

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“…These variants, named expression quantitative trait loci (eQTL), provide a functional relevance for the association between genetic variants and AIDs. The eQTL analysis was recently applied to rheumatoid arthritis (RA) and successfully predicted the importance of the tumor necrosis factor (TNF) pathway in CD4 + T cells . Although eQTLs have never been studied directly for MG, a screen of cis ‐eQTLs for 353 AID risk variants in 42 human thymic tissues identified eight eQTLs associated with seven genetic regions, including two regions that were thymus specific .…”

Section: Typical Molecular Signatures In Mg and Other Aidsmentioning

confidence: 99%

Pathophysiological mechanisms of autoimmunity

Sudres

Verdier

Truffault

et al. 2018

Annals of the New York Academy of Sciences

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Autoimmune diseases (AIDs) are chronic disorders characterized by inflammatory reactions against self-antigens that can be either systemic or organ specific. AIDs can differ in their epidemiologic features and clinical presentations, yet all share a remarkable complexity. AIDs result from an interplay of genetic and epigenetic factors with environmental components that are associated with imbalances in the immune system. Many of the pathogenic mechanisms of AIDs are also implicated in myasthenia gravis (MG), an AID in which inflammation of the thymus leads to a neuromuscular disorder. Our goal here is to highlight the similarities and differences between MG and other AIDs by reviewing the common transcriptome signatures and the development of germinal centers and by discussing some unresolved questions about autoimmune mechanisms. This review will propose hypotheses to explain the origin of regulatory T (T ) cell defects and the causes of chronicity and specificity of AIDs.

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Polygenic burdens on cell-specific pathways underlie the risk of rheumatoid arthritis

Cited by 127 publications

References 39 publications

Reduction of CD83 Expression on B Cells and the Genetic Basis for Rheumatoid Arthritis: Comment on the Article by Thalayasingam et al

Reduction of CD83 Expression on B Cells and the Genetic Basis for Rheumatoid Arthritis: Comment on the Article by Thalayasingam et al

Ch IP ‐Atlas: a data‐mining suite powered by full integration of public Ch IP ‐seq data

Pathophysiological mechanisms of autoimmunity

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