Developments in the prediction of type 1 diabetes mellitus, with special reference to insulin autoantibodies

Franke, Bernd; Galloway, Tamara S.; Wilkin, Terry

doi:10.1002/dmrr.554

Cited by 29 publications

(24 citation statements)

References 246 publications

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“…Half of these (7/14) seroconverted before they were 9 months old, including two before 6 months of age. IAA and anti-GAD were the first islet autoantibodies to appear, with anti-IA2 appearing closer to the onset of type 1 diabetes, consistent with previous studies [13,33]. In the same group of children, presence of type 1 diabetes in a first-degree relative was associated with significantly higher risk of islet autoimmunity, confirming other studies [34,35].…”

Section: Discussionsupporting

confidence: 91%

Islet autoantibody development during follow-up of high-risk children from the general Norwegian population from three months of age: Design and early results from the MIDIA study

Stene

Witsø

Torjesen

et al. 2007

Journal of Autoimmunity

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Section: Discussionsupporting

confidence: 91%

Islet autoantibody development during follow-up of high-risk children from the general Norwegian population from three months of age: Design and early results from the MIDIA study

Stene

Witsø

Torjesen

et al. 2007

Journal of Autoimmunity

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“…Moreover, the anti-tTG antibodies do not seem to contribute to the formation of the intestinal lesions in CD because disease symptoms disappear rapidly after the introduction of a gluten-free diet and antibody titers drop much slower. Similarly, in type I diabetes autoantibodies against islet cells, glutamic acid decarboxylase, protein-tyrosine phosphatase-2, and insulin can be found, which might reflect the ongoing autoimmune process, but most likely do not participate in the tissue damage [52].…”

Section: Autoantibodies To Tissue Transglutaminase Are Specific Indicmentioning

confidence: 99%

Celiac Disease—Sandwiched between Innate and Adaptive Immunity

2006

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“…Clinical onset is often preceded by the presence of islet cell autoantibodies that are useful for predicting T1DM (1)(2)(3). Risk estimates vary, however; a titer for a single autoantibody among first-degree relatives imparts little risk, whereas high titers for two or three Abs are predictive (Ͼ80%) of disease within 5 years (4,5). T1DM patients have an estimated 80 -90% loss in ␤ cell mass at diagnosis, although functioning mass still remains (6).…”

Section: T Ype 1 Diabetes Mellitus (T1dm)mentioning

confidence: 99%

Identification of a Molecular Signature in Human Type 1 Diabetes Mellitus Using Serum and Functional Genomics

Wang

Song

Geoffrey

et al. 2008

The Journal of Immunology

103

156

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Understanding active proinflammatory mechanisms at and before type 1 diabetes mellitus (T1DM) onset is hindered in humans, given that the relevant tissues are inaccessible and pancreatic immune responses are difficult to measure in the periphery by traditional approaches. Therefore, we investigated the use of a sensitive and comprehensive genomics strategy to investigate the presence of proinflammatory factors in serum. The sera of recent onset diabetes patients (n = 15, 12 possessing and 3 lacking islet cell autoantibodies), long-standing diabetes patients (n = 12), “at risk” siblings of diabetes patients (n = 9), and healthy controls (n = 12) were used to induce gene expression in unrelated, healthy PBMC. After culture, gene expression was measured with microarrays and normalized expression data were subjected to hierarchical clustering and multidimensional scaling. All recent onset sera induced an expression signature (192 UniGenes; fold change: >1.5, p < 0.01; false discovery rate: <0.01) that included IL-1 cytokine family members and chemokines involved in monocyte/macrophage and neutrophil chemotaxis, as well as numerous receptors and signaling molecules. This molecular signature was not induced with the sera of healthy controls or long standing diabetes patients, where longitudinal analysis of “at risk” siblings (n = 3) before and after onset support the hypothesis that the signature emerges years before onset. This study supports prior investigations of serum that reflect disease processes associated with progression to T1DM. Identification of unique inflammatory mediators may improve disease prediction beyond current islet autoantibodies. Furthermore, proinflammatory serum markers may be used as inclusion criteria or endpoint measures in clinical trials aimed at preventing T1DM.

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Developments in the prediction of type 1 diabetes mellitus, with special reference to insulin autoantibodies

Cited by 29 publications

References 246 publications

Islet autoantibody development during follow-up of high-risk children from the general Norwegian population from three months of age: Design and early results from the MIDIA study

Islet autoantibody development during follow-up of high-risk children from the general Norwegian population from three months of age: Design and early results from the MIDIA study

Celiac Disease—Sandwiched between Innate and Adaptive Immunity

Identification of a Molecular Signature in Human Type 1 Diabetes Mellitus Using Serum and Functional Genomics

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