The genetic and regulatory architecture of ERBB3-type 1 diabetes susceptibility locus

Kaur, Simranjeet; Mirza, Aashiq H.; Brorsson, Caroline; Fløyel, Tina; Størling, Joachim; Mortensen, Henrik B.; Pociot, Flemming

doi:10.1016/j.mce.2015.10.002

Cited by 31 publications

(20 citation statements)

References 53 publications

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“…The most robust association was reported with the Erb‐B2 Receptor Tyrosine Kinase 3 (ERBB3) rs2292239 T1D risk SNP and HbA1c level. The association remains significant after adjusting for insulin dose, gender, age at onset, and diabetes duration, but this finding has not been replicated yet. The Protein Tyrosine Phosphatase Non‐receptor type 22 (PTPN22) T1D risk allele was associated with HbA1c level, but this finding was not replicated in an independent study that used the insulin dose‐adjusted HbA1c measure (IDAAC), defined by Mortensen et al in 2009 .…”

Section: Resultsmentioning

confidence: 79%

“…These candidate gene association studies have never been or have been poorly replicated, except for angiotensin I converting enzyme (ACE) gene . Five of the 13 selected studies reported significant or suggestive associations, which were however never replicated …”

Section: Resultsmentioning

confidence: 99%

“…[129][130][131] Five of the 13 selected studies reported significant or suggestive associations, which were however never replicated. 120,123,124,126,128 The most robust association was reported with the Erb-B2 Receptor Tyrosine Kinase 3 (ERBB3) rs2292239 T1D risk SNP and HbA1c level. The association remains significant after adjusting for insulin dose, gender, age at onset, and diabetes duration, 128…”

Section: Candidate Gene Studiesmentioning

confidence: 99%

“…120,123,124,126,128 The most robust association was reported with the Erb-B2 Receptor Tyrosine Kinase 3 (ERBB3) rs2292239 T1D risk SNP and HbA1c level. The association remains significant after adjusting for insulin dose, gender, age at onset, and diabetes duration, 128…”

Section: Candidate Gene Studiesmentioning

confidence: 99%

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A systematic review of non‐genetic predictors and genetic factors of glycated haemoglobin in type 1 diabetes one year after diagnosis

Gloaguen

Bendelac

Nicolino

et al. 2018

Diabetes Metabolism Res

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Type 1 diabetes (T1D) results from autoimmune destruction of the pancreatic βcells. Although all T1D patients require daily administration of exogenous insulin, their insulin requirement to achieve good glycaemic control may vary significantly. Glycated haemoglobin (HbA1c) level represents a stable indicator of glycaemic control and is a reliable predictor of long-term complications of T1D. The purpose of this article is to systematically review the role of non-genetic predictors and genetic factors of HbA1c level in T1D patients after the first year of T1D, to exclude the honeymoon period. A total of 1974 articles published since January 2011 were identified and 78 were finally included in the analysis of non-genetic predictors. For genetic factors, a total of 277 articles were identified and 14 were included. The most significantly associated factors with HbA1c level are demographic (age, ethnicity, and socioeconomic status), personal (family characteristics, parental care, psychological traits...) and features related to T1D (duration of T1D, adherence to treatment …). Only a few studies have searched for genetic factors influencing HbA1c level, most of which focused on candidate genes using classical genetic statistical methods, with generally limited power and incomplete adjustment for confounding factors and multiple testing. Our review shows the complexity of explaining HbA1c level variations, which involves numerous correlated predictors. Overall, our review underlines the lack of studies investigating jointly genetic and non-genetic factors and their interactions to better understand factors influencing glycaemic control for T1D patients.

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Section: Resultsmentioning

confidence: 79%

Section: Resultsmentioning

confidence: 99%

Section: Candidate Gene Studiesmentioning

confidence: 99%

Section: Candidate Gene Studiesmentioning

confidence: 99%

See 2 more Smart Citations

A systematic review of non‐genetic predictors and genetic factors of glycated haemoglobin in type 1 diabetes one year after diagnosis

Gloaguen

Bendelac

Nicolino

et al. 2018

Diabetes Metabolism Res

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“…rs4759229 is in perfect LD with T1D risk SNP rs2292239, overlaps a known enhancer region and has a long range interaction signal with an antisense lncRNA AC008079.1 (Ensembl ID: ENSG00000187979) located at USP18 locus on chromosome 22. In a recent study, we proposed that the ERBB3 SNP rs2292239 and its proxy SNPs in perfect LD rs3741499 and rs4759229 are putatively functional based on the overlapping open chromatin marks, TFBs and DNase I hypersensitivity peaks [79]. We further showed that SNP rs4759229 overlaps a known enhancer element and is in the vicinity of several lncRNA transcripts overlapping ERBB3 locus.…”

Section: Main Textmentioning

confidence: 99%

Long non-coding RNAs as novel players in β cell function and type 1 diabetes

2017

Self Cite

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BackgroundLong non-coding RNAs (lncRNAs) are a sub-class within non-coding RNA repertoire that have emerged as crucial regulators of the gene expression in various pathophysiological conditions. lncRNAs display remarkable versatility and wield their functions through interactions with RNA, DNA, or proteins. Accumulating body of evidence based on multitude studies has highlighted the role of lncRNAs in many autoimmune and inflammatory diseases, including type 1 diabetes (T1D).Main body of abstractThis review highlights emerging roles of lncRNAs in immune and islet β cell function as well as some of the challenges and opportunities in understanding the pathogenesis of T1D and its complications.ConclusionWe accentuate that the lncRNAs within T1D-loci regions in consort with regulatory variants and enhancer clusters orchestrate the chromatin remodeling in β cells and thereby act as cis/trans-regulatory determinants of islet cell transcriptional programs.

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Genetic variation at ERBB3/IKZF4 and sexual dimorphism in epitope spreading in single autoantibody-positive relatives

et al. 2021

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Aims/hypothesis We examined whether the non-HLA susceptibility locus ERBB3/IKZF4 influences progression of type 1 diabetes stage specifically according to sex. Methods SNPs of ERBB3 (rs2292239 T/G) and IKZF4 (rs1701704 G/T) were screened by allelic discrimination quantitative PCR assay in first-degree relatives of type 1 diabetes patients who had developed at least one circulating autoantibody. The effect of ERBB3/IKZF4 genotypes and sex, on the progression of single autoantibody positivity to multiple autoantibody positivity and from multiple autoantibody positivity to diabetes, was studied by Kaplan–Meier analysis and multivariate Cox regression. Results In the cohort of autoantibody-positive first-degree relatives, the risk allele frequencies for ERBB3 rs2292239 (T) and IKZF4 rs1701704 (G) were increased. There was a significant male excess at the stage of multiple autoantibody positivity (p = 0.021). In Kaplan–Meier survival analysis, progression from single to multiple antibody positivity was delayed in female participants with genotype ERBB3 GG (p = 0.018, vs ERBB3 TG+TT) or IKZF4 TT (p = 0.023, vs IKZF4 GT+GG), but not in male participants. In multivariate Cox regression models, the interaction effects between female sex and ERBB3 GG (p = 0.012; HR = 0.305 [95% CI 0.120, 0.773]) or between female sex and IKZF4 TT (p = 0.011; HR = 0.329 [95% CI 0.140, 0.777]) emerged as potential determinants of delayed progression to multiple autoantibodies. The progression from multiple autoantibody positivity to type 1 diabetes appeared not to be influenced by ERBB3/IKZF4. Conclusions/interpretation In siblings and offspring of type 1 diabetes patients, polymorphism in region ERBB3/IKZF4 may affect disease progression at the level of epitope spreading in female individuals. Our findings suggest that interaction between sex and ERBB3/IKZF4 may contribute to the post-pubertal male excess in type 1 diabetes. Graphical abstract

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The genetic and regulatory architecture of ERBB3-type 1 diabetes susceptibility locus

Cited by 31 publications

References 53 publications

A systematic review of non‐genetic predictors and genetic factors of glycated haemoglobin in type 1 diabetes one year after diagnosis

A systematic review of non‐genetic predictors and genetic factors of glycated haemoglobin in type 1 diabetes one year after diagnosis

Long non-coding RNAs as novel players in β cell function and type 1 diabetes

Genetic variation at ERBB3/IKZF4 and sexual dimorphism in epitope spreading in single autoantibody-positive relatives

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