Your search keyword '"Koeleman, B. P. C."' showing total 6 results

1. Post-transcriptional control of candidate risk genes for type 1 diabetes by rare genetic variants.

Author

de Jong, V M, Zaldumbide, A, van der Slik, A R, Persengiev, S P, Roep, B O, and Koeleman, B P C

Subjects

DIABETES risk factors, DISEASE susceptibility, MICRORNA, BINDING sites, MESSENGER RNA, IMMUNOREGULATION

Abstract

The genetic variation causal for predisposition to type 1 diabetes (T1D) remains unidentified for the majority of known T1D risk loci. MicroRNAs function as post-transcriptional gene regulators by targeting microRNA-binding sites in the 3′ untranslated regions (UTR) of mRNA. Genetic variation within the 3′-UTR of T1D-associated genes may contribute to T1D development by altering microRNA-mediated gene regulation. In silico analysis of variable sites predicted altered microRNA binding in established T1D loci. Functional implications were assessed for variable sites in the 3′-UTR of T1D candidate risk genes CTLA4 and IL10, both involved in immune regulation. We confirmed that in these genes 3′-UTR variation either disrupted or introduced a microRNA-binding site, affecting the repressive capacity of miR-302a* and miR-523, respectively. Our study points to the potential of 3′-UTR variation to affect T1D pathogenesis by altering post-transcriptional gene regulation by microRNAs. [ABSTRACT FROM AUTHOR]

Published

2013

2. Functional consequences of HLA-DQ8 homozygosity versus heterozygosity for islet autoimmunity in type 1 diabetes.

Author

Eerligh, P, van Lummel, M, Zaldumbide, A, Moustakas, A K, Duinkerken, G, Bondinas, G, Koeleman, B P C, Papadopoulos, G K, and Roep, B O

Subjects

GENETICS of diabetes, HLA class II antigens, AUTOIMMUNITY, EPITOPES, PROTEIN binding, ANTI-inflammatory agents, IMMUNE response

Abstract

Human leukocyte antigen (HLA) class II haplotypes are established risk factors in type 1 diabetes (T1D). The heterozygous DQ2/8 genotype confers the highest risk, whereas the DQ6/8 genotype is protective. We hypothesized that DQ2/8 trans-molecules composed of α and β chains from DQ2 and DQ8 express unique β-cell epitopes, whereas DQ6 may interfere with peptide binding to DQ8. Here we show that a single insulin epitope (InsB13-21) within the T1D prototype antigenic InsB6-22 peptide can bind to both cis- and trans-dimers, although these molecules display different peptide binding patterns. DQ6 binds a distinct insulin epitope (InsB6-14). The phenotype of DQ8-restricted T cells from a T1D patient changed from proinflammatory to anti-inflammatory in the presence of DQ6. Our data provide new insights into both susceptible and protective mechanism of DQ, where protecting HLA molecules bind autoantigens in a different (competing) binding register leading to 'epitope stealing', thereby inducing a regulatory, rather than a pathogenic immune response. [ABSTRACT FROM AUTHOR]

Published

2011

3. Genetic variants of RANTES are associated with serum RANTES level and protection for type 1 diabetes.

Author

Zhernakova, A., Alizadeh, B. Z., Eerligh, P., Hanifi-Moghaddam, P., Schloot, N. C., Diosdado, B., Wijmenga, C., Roep, B. O., and Koeleman, B. P. C.

Subjects

GENETICS of diabetes, T cells, CHEMOKINES, AUTOIMMUNE diseases, GENETIC polymorphisms, CELL proliferation, CHROMOSOMES, MEDICAL genetics

Abstract

RANTES (regulated on activation, normal T-cell expressed and secreted) is a T-helper type 1 (Th1) chemokine that promotes T-cell activation and proliferation. RANTES is genetically associated with asthma, sarcoidosis and multiple sclerosis. The concentration of RANTES is increased at inflammation sites in different autoimmune diseases. Type 1 diabetes (T1D) is a Th1-mediated disease with complex genetic predisposition. We tested RANTES as a candidate gene for association with T1D using three single-nucleotide polymorphism (SNP) variants (rs4251719, rs2306630 and rs2107538) to capture haplotype information. The minor alleles of all SNPs were transmitted less frequently to T1D offspring (transmission rates 37.3% (P=0.002), 38.7% (P=0.007) and 41.0% (P=0.01)) and were less frequently present in patients compared to controls (P=0.009, 0.03 and 0.04, respectively). A similar protective effect was observed for the haplotype carrying three minor alleles (transmission disequilibrium test (TDT): P=0.003; odds ratio (OR)=0.55; confidence interval (CI): 0.37–0.83; case/control: P=0.03; OR=0.74; CI: 0.55–0.98). Both patients and controls carrying the protective haplotype express significantly lower serum levels of RANTES compared to non-carriers. Subsequently, we tested a cohort of 310 celiac disease patients, but failed to detect association. RANTES SNPs are significantly associated with RANTES serum concentration and development of T1D. The rs4251719*A–rs2306630*A–rs2107538*A haplotype associated with low RANTES production confers protection from T1D. Our data imply that RANTES is associated with T1D both genetically and functionally, and contributes to diabetes-prone Th1 cytokine profile.Genes and Immunity (2006) 7, 544–549. doi:10.1038/sj.gene.6364326; published online 20 July 2006 [ABSTRACT FROM AUTHOR]

Published

2006

4. Genotype effects and epistasis in type 1 diabetes and HLA-DQ trans dimer associations with disease.

Author

Koeleman, B. P. C., Lie, B. A., Undlien, D. E., Dudbridge, F., Thorsby, E., de Vries, R. R. P., Cucca, F., Roep, B. O., Giphart, M. J., and Todd, J. A.

Subjects

*EPISTASIS (Genetics), *MOLECULES, *IMMUNITY, *DISEASES

Abstract

Alleles of HLA class II genes DQB1, DQA1, and DRB1 in the MHC region are major determinants of genetic predisposition to type 1 diabetes (T1D). Several alleles of each of these three loci are associated with susceptibility or protection from disease. In addition, relative risks for some DR-DQ genotypes are not simply the sum or product of the single haplotype relative risks. For example, the risk of the DRB1*03-DQB1*02/DRB1*0401-DQB1*0302 genotype is often found to be higher than for the individual DRB1*03-DQB1*02 and DRB1*0401-DQB1*0302 homozygous genotypes. It has been hypothesized that this synergy or epistasis occurs through formation of highly susceptible trans-encoded HLA-DQ(a1, ß1) heterodimers. Here, we evaluated this hypothesis by estimating the disease associations of the range of DR-DQ genotypes and their inferred dimers in a large collection of nuclear families. We determined whether the risk of haplotypes in DRB1*0401-DQB1*0302-positive genotypes relative to the DRB1*03-DQB1*02-positive genotypes is different from that of DRB1*01-DQB1*0501, which we used as a baseline reference. Several haplotypes showed a different risk compared to DRB1*01-DQB1*0501, which correlated with their ability to form certain trans-encoded DQ dimers. This result provides new evidence for the potential importance of trans-encoded HLA DQ molecules in the determination of HLA-associated risk in T1D.Genes and Immunity (2004) 5, 381-388. doi:10.1038/sj.gene.6364106 Published online 27 May 2004 [ABSTRACT FROM AUTHOR]

Published

2004

5. Defining the contribution of the HLA region to cis DQ2-positive coeliac disease patients.

Author

van Belzen, M. J., Koeleman, B. P. C., Crusius, J. B. A., Meijer, J. W. R., Bardoel, A. F. J., Pearson, P. L., Sandkuijl, L. A., Houwen, R. H. J., and Wijmenga, C.

Subjects

*CELIAC disease, *HLA histocompatibility antigens, *GENES, *LINKAGE (Genetics), *GENETICS, *IMMUNITY

Abstract

The major genetic susceptibility to coeliac disease is contributed by the human leukocyte antigen (HLA) region. The primary association is with the HLA-DQ2 molecule, encoded by the DQA1*05 and DQB1*02 alleles, which is expressed by over 90% of patients. The aim of our study was to perform an extensive scan of the entire HLA region to determine whether there is evidence for the presence of additional HLA susceptibility genes for coeliac disease in the Dutch population, acting independently of DQ2. In all, 16 microsatellite markers and the DQA1 and DQB1 genes were genotyped in simplex cis DQ2-positive coeliac disease families and cis DQ2-positive control families. Allele frequencies of markers on phase-known DQ2-positive haplotypes transmitted to patients were compared to a combined group of DQ2-positive nontransmitted and control haplotypes, thereby controlling for the DQ2 contribution. No significant differences at any of the marker loci were detected, suggesting that DQ2 is the major HLA risk factor for coeliac disease. Individuals homozygous for DQ2 or heterozygous for DQA1*05-DQB1*02/DQA1*0201-DQB1*02 were found to be at five-fold increased risk for development of coeliac disease (P<10-8). This risk seems to be conferred by the presence of a second DQB1*02 allele next to one DQA1*05-DQB1*02 haplotype, independently of the second DQA1 allele.Genes and Immunity (2004) 5, 215-220. doi:10.1038/sj.gene.6364061 Published online 11 March 2004 [ABSTRACT FROM AUTHOR]

Published

2004

6. Differential association of the PTPN22 coding variant with autoimmune diseases in a Dutch population.

Author

Zhernakova, A., Eerligh, P., Wijmenga, C., Barrera, P., Roep, B. O., and Koeleman, B. P. C.

Subjects

AUTOIMMUNE diseases, DIABETES, ARTHRITIS, PROTEIN-tyrosine phosphatase, BLOOD hyperviscosity syndrome

Abstract

Protein tyrosine phosphatase PTPN22 is involved in the negative regulation of T-cell responsiveness. Recently, the association of a coding variant of the PTPN22 gene-R620W(1858C>T) with a number of autoimmune diseases has been described. Therefore, we tested the association of PTPN22 1858*T allele in Dutch early onset type 1 diabetes (T1D) and rheumatoid arthritis (RA) patients, as well as celiac disease (CD) patients, for which no previous study of PTPN22 has been reported. The PTPN22 variant was strongly associated with T1D in cases vs controls (P=2 × 10−7, OR=2.3, 95% CI=1.7–3.1) as well as in a transmission disequilibrium test in nuclear trio's (P=9 × 10−9, OR=3.3, CI=2.1–5.0), RA (case/control: P=0.003, OR=1.8 CI =1.2–2.6), but not CD, in spite of a trend of increased homozygosity (P=0.05) and early age at onset (P=0.01). PTPN22 is not generally associated with T-cell mediated autoimmune diseases, although it might play a role in the CD patients with early clinical manifestation.Genes and Immunity (2005) 6, 459–461. doi:10.1038/sj.gene.6364220; published online 5 May 2005 [ABSTRACT FROM AUTHOR]

Published

2005