Dendritic Cells Guide Islet Autoimmunity through a Restricted and Uniquely Processed Peptidome Presented by High-Risk HLA-DR

Lummel, Menno van; Veelen, Peter A. van; Ru, Arnoud H. de; Janssen, George M.C.; Pool, J.; Laban, Sandra; Joosten, Antoinette M.; Nikolić, Tatjana; Drijfhout, Jan W.; Aanstoot, Henk‐Jan; Peakman, Mark; Roep, Bart O.

doi:10.4049/jimmunol.1501282

Cited by 26 publications

(15 citation statements)

References 57 publications

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“…Although T1D is classified as a Group I disease, until recently it was not recognized to have pathogenic autoantibodies. However, newer information suggests that IA2, a cell surface molecule, is a target of B- and T-cell responses [52, 53] and may be involved in pathogenesis. It is also possible that transcriptomic analysis could be used to identify novel candidate autoantigens in Group I disorders.…”

Section: Discussionmentioning

confidence: 99%

“…Two other targets, IA2 and IA2β are cell surface proteins containing both extracellular and intracellular regions, which are encoded by 950 and 977 amino acids, respectively. Interestingly, recent evidence suggests that IA2 is a target of B- and T-cell responses [52, 53] and may be involved in T1D pathogenesis. ZnT8 is a transmembrane protein of 369 amino acids found on intracellular vesicles.…”

Section: Autoimmune Disease Overview Along With the Corresponding Dmentioning

confidence: 99%

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Transcriptomic Segregation of Human Autoantigens Useful for the Diagnosis of Autoimmune Diseases

et al. 2016

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The measurement of autoantibodies in the clinical care of autoimmune patients allows for diagnosis, monitoring, and even disease prediction. Despite their clinical utility, the functional significance of autoantibody target proteins in many autoimmune diseases remains unclear. Here we present a comprehensive review of 52 autoantigens commonly employed for the serological diagnosis of 24 autoimmune diseases. We discuss their function, whether they have extracellular-exposed epitopes, and whether antibodies to these proteins are known to be pathogenic. Transcriptomics (RNA-Seq) datasets were mined to display messenger RNA (mRNA) expression of the autoantigens across 32 tissues and organs. This analysis revealed that autoantigens cluster into one of three groups: expression in the tissue most strongly affected in the disease (Group I), ubiquitous expression with enrichment in immune tissues (Group II), or expression in other tissues not typically associated with the clinical presentation (Group III). Clustering demonstrated that the autoantigens within Group I were often proteins containing extracellular epitopes, many of which are targets of pathogenic autoantibodies. Group II autoantigens were targets for several rheumatological diseases, including Sjögren syndrome, systemic lupus erythematosus, myositis, and systemic sclerosis, and were ubiquitously expressed with enrichment in immune-rich tissues. This raises the possibility that immune cells in Group II disorders may be the source of autoimmunization and/or targets of immune cell responses. Since tissues showing enriched autoantigen gene expression may contribute to the development of autoantibodies and subsequent autoimmunity, the emergent patterns arising from the autoantigen transcriptomic profiles may provide a new heuristic framework to deconvolute these complex disorders.

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Section: Discussionmentioning

confidence: 99%

Section: Autoimmune Disease Overview Along With the Corresponding Dmentioning

confidence: 99%

Transcriptomic Segregation of Human Autoantigens Useful for the Diagnosis of Autoimmune Diseases

et al. 2016

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“…These dendritic cells are able to present MHC class I and II molecules and prompt effector leukocytes infiltration through a Batf3 depending pathway, which conduce to the autoimmunity progress against mice islet cells 68 . In addition, an investigation on human high risk HLA‐DR molecules indicated dendritic cells are capable of presenting islet epitopes bound with susceptible HLA‐DR molecules, which manifest the crucial initiator role of dendritic cells in islet autoimmunity 70 . However, no investigation on dendritic cells functioning in FT1D patients was reported up to now.…”

Section: Antigen Presenting Cells and Pattern Recognition Receptors Amentioning

confidence: 99%

Fulminant type 1 diabetes: A comprehensive review of an autoimmune condition

Luo

et al. 2020

Diabetes Metabolism Res

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Summary Fulminant type 1 diabetes (FT1D) is a subset of type 1 diabetes characterized by extremely rapid pancreatic β‐cell destruction with aggressive progression of hyperglycaemia and ketoacidosis. It was initially classified as idiopathic type 1 diabetes due to the absence of autoimmune markers. However, subsequent studies provide evidences supporting the involvement of autoimmunity in rapid β‐cell loss in FT1D pathogenesis, which are crucial for FT1D being an autoimmune disease. This article highlights the role of immunological aspects in FT1D according to the autoimmune‐associated genetic background, viral infection, innate immunity, adaptive immunity, and pancreas histology.

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“…B lymphocytes are reported to be present in small numbers in early insulitis but are recruited to islets as beta cell death progresses, suggesting that they are a consequence, rather than cause, of insulitis [13]. B lymphocytes take up and process antigens in a concentration-dependent manner and are more than a thousand times less efficient than dendritic cells at presenting antigens if they do not happen to express the B cell receptor for a particular islet autoantigen [14]. For B lymphocytes to get involved, they must first be activated by T cells that are primed prior to seroconversion.…”

Section: B Lymphocytes In Type 1 Diabetesmentioning

confidence: 99%

The elusive role of B lymphocytes and islet autoantibodies in (human) type 1 diabetes

Bloem

Roep

2017

Diabetologia

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The role of B lymphocytes in the pathogenesis of type 1 diabetes in humans is not entirely evident. These cells are presumed to be important, but this assumption is largely based on animal models of autoimmune diabetes, where compelling evidence for the contribution of both B lymphocytes and insulin-specific autoantibodies to this disease is in place. For humans, this is much less the case; the exact way in which B lymphocytes and/or autoantibodies may contribute to type 1 diabetes is not yet known but the possibilities include a pathogenic function ('fire'), or they may represent a surrogate of loss of immune tolerance to beta cells ('smoke') or, indeed, they could be a marker of an attempt at immune regulation ('ice water'). In this issue of Diabetologia, a study by Willcox et al (DOI: 10.1007/s00125-017-4221-7) adds new information but no greater clarity on the relevance of B lymphocytes in type 1 diabetes, showing a decrease in germinal centre frequencies in donors with recent-onset type 1 diabetes compared with control donors and donors with longstanding type 1 diabetes. These new findings may guide the research community to design experiments to unambiguously define whether B lymphocytes or their products function as fire, smoke or perhaps ice water in the immunopathogenesis of type 1 diabetes.

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Dendritic Cells Guide Islet Autoimmunity through a Restricted and Uniquely Processed Peptidome Presented by High-Risk HLA-DR

Cited by 26 publications

References 57 publications

Transcriptomic Segregation of Human Autoantigens Useful for the Diagnosis of Autoimmune Diseases

Transcriptomic Segregation of Human Autoantigens Useful for the Diagnosis of Autoimmune Diseases

Fulminant type 1 diabetes: A comprehensive review of an autoimmune condition

The elusive role of B lymphocytes and islet autoantibodies in (human) type 1 diabetes

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