Your search keyword '"Stevens, Helen E"' showing total 4 results

1. Localization of type 1 diabetes susceptibility to the MHC class I genes HLA-B and HLA-A.

Author

Nejentsev, Sergey, Howson, Joanna M. M., Walker, Neil M., Szeszko, Jeffrey, Field, Sarah F., Stevens, Helen E., Reynolds, Pamela, Hardy, Matthew, King, Erna, Masters, Jennifer, Hulme, John, Maier, Lisa M., Smyth, Deborah, Bailey, Rebecca, Cooper, Jason D., Ribas, Gloria, Campbell, R. Duncan, Clayton, David G., and Todd, John A.

Subjects

DIABETES, MAJOR histocompatibility complex, CHROMOSOMES, GENES, GENETIC polymorphisms, HUMAN genome, AUTOIMMUNE diseases, PROPERTIES of matter, STATISTICS

Abstract

The major histocompatibility complex (MHC) on chromosome 6 is associated with susceptibility to more common diseases than any other region of the human genome, including almost all disorders classified as autoimmune. In type 1 diabetes the major genetic susceptibility determinants have been mapped to the MHC class II genes HLA-DQB1 and HLA-DRB1 (refs 1–3), but these genes cannot completely explain the association between type 1 diabetes and the MHC region. Owing to the region’s extreme gene density, the multiplicity of disease-associated alleles, strong associations between alleles, limited genotyping capability, and inadequate statistical approaches and sample sizes, which, and how many, loci within the MHC determine susceptibility remains unclear. Here, in several large type 1 diabetes data sets, we analyse a combined total of 1,729 polymorphisms, and apply statistical methods—recursive partitioning and regression—to pinpoint disease susceptibility to the MHC class I genes HLA-B and HLA-A (risk ratios >1.5; Pcombined = 2.01 × 10-19 and 2.35 × 10-13, respectively) in addition to the established associations of the MHC class II genes. Other loci with smaller and/or rarer effects might also be involved, but to find these, future searches must take into account both the HLA class II and class I genes and use even larger samples. Taken together with previous studies, we conclude that MHC-class-I-mediated events, principally involving HLA-B*39, contribute to the aetiology of type 1 diabetes. [ABSTRACT FROM AUTHOR]

Published

2007

2. Robust associations of four new chromosome regions from genome-wide analyses of type 1 diabetes.

Author

Todd, John A., Walker, Neil M., Cooper, Jason D., Smyth, Deborah J., Downes, Kate, Plagnol, Vincent, Bailey, Rebecca, Nejentsev, Sergey, Field, Sarah F., Payne, Felicity, Lowe, Christopher E., Szeszko, Jeffrey S., Hafler, Jason P., Zeitels, Lauren, Yang, Jennie H. M., Vella, Adrian, Nutland, Sarah, Stevens, Helen E., Schuilenburg, Helen, and Coleman, Gillian

Subjects

GENOMICS, DIABETES, AUTOIMMUNE diseases, GENETIC polymorphisms, GENETICS of disease susceptibility, THYROID diseases, GRAVES' disease

Abstract

The Wellcome Trust Case Control Consortium (WTCCC) primary genome-wide association (GWA) scan on seven diseases, including the multifactorial autoimmune disease type 1 diabetes (T1D), shows associations at P < 5 × 10−7 between T1D and six chromosome regions: 12q24, 12q13, 16p13, 18p11, 12p13 and 4q27. Here, we attempted to validate these and six other top findings in 4,000 individuals with T1D, 5,000 controls and 2,997 family trios independent of the WTCCC study. We confirmed unequivocally the associations of 12q24, 12q13, 16p13 and 18p11 (Pfollow-up ≤ 1.35 × 10−9; Poverall ≤ 1.15 × 10−14), leaving eight regions with small effects or false-positive associations. We also obtained evidence for chromosome 18q22 (Poverall = 1.38 × 10−8) from a GWA study of nonsynonymous SNPs. Several regions, including 18q22 and 18p11, showed association with autoimmune thyroid disease. This study increases the number of T1D loci with compelling evidence from six to at least ten. [ABSTRACT FROM AUTHOR]

Published

2007

3. Population structure, differential bias and genomic control in a large-scale, case-control association study.

Author

Clayton, David G., Walker, Neil M., Smyth, Deborah J., Pask, Rebecca, Cooper, Jason D., Maier, Lisa M., Smink, Luc J., Lam, Alex C., Ovington, Nigel R., Stevens, Helen E., Nutland, Sarah, Howson, Joanna M. M., Faham, Malek, Moorhead, Martin, Jones, Hywel B., Falkowski, Matthew, Hardenbol, Paul, Willis, Thomas D., and Todd, John A.

Subjects

GENOMICS, GENETICS, GENETIC research, GENETIC polymorphisms, POPULATION genetics

Abstract

The main problems in drawing causal inferences from epidemiological case-control studies are confounding by unmeasured extraneous factors, selection bias and differential misclassification of exposure. In genetics the first of these, in the form of population structure, has dominated recent debate. Population structure explained part of the significant +11.2% inflation of test statistics we observed in an analysis of 6,322 nonsynonymous SNPs in 816 cases of type 1 diabetes and 877 population-based controls from Great Britain. The remainder of the inflation resulted from differential bias in genotype scoring between case and control DNA samples, which originated from two laboratories, causing false-positive associations. To avoid excluding SNPs and losing valuable information, we extended the genomic control method by applying a variable downweighting to each SNP. [ABSTRACT FROM AUTHOR]

Published

2005

4. Plasma concentrations of soluble IL-2 receptor α (CD25) are increased in type 1 diabetes and associated with reduced C-peptide levels in young patients

Author

Downes, Kate, Marcovecchio, M Loredana, Clarke, Pamela, Cooper, Jason D, Ferreira, Ricardo C, Howson, Joanna MM, Jolley, Jennifer, Nutland, Sarah, Stevens, Helen E, Walker, Neil M, Wallace, Chris, Dunger, David B, Todd, John A, Downes, Kate [0000-0003-0366-1579], Marcovecchio, Loredana [0000-0002-4415-316X], Howson, Joanna [0000-0001-7618-0050], Wallace, Chris [0000-0001-9755-1703], Dunger, David [0000-0002-2566-9304], and Apollo - University of Cambridge Repository

Subjects

Adult, Immunoassay, Inflammation, Male, Adolescent, C-Peptide, Endocrinology, Diabetes and Metabolism, Interleukin-2 Receptor alpha Subunit, Middle Aged, Diabetes Mellitus, Type 1, Case-Control Studies, Insulin-Secreting Cells, Disease Progression, Internal Medicine, Humans, Female, Biomarkers, Aged

Abstract

AIMS/HYPOTHESIS: Type 1 diabetes is a common autoimmune disease that has genetic and environmental determinants. Variations within the IL2 and IL2RA (also known as CD25) gene regions are associated with disease risk, and variation in expression or function of these proteins is likely to be causal. We aimed to investigate if circulating concentrations of the soluble form of CD25, sCD25, an established marker of immune activation and inflammation, were increased in individuals with type 1 diabetes and if this was associated with the concentration of C-peptide, a measure of insulin production that reflects the degree of autoimmune destruction of the insulin-producing beta cells. METHODS: We used immunoassays to measure sCD25 and C-peptide in peripheral blood plasma from patient and control samples. RESULTS: We identified that sCD25 was increased in patients with type 1 diabetes compared with controls and replicated this result in an independent set of 86 adult patient and 80 age-matched control samples (p = 1.17 × 10(-3)). In 230 patients under 20 years of age, with median duration-of-disease of 6.1 years, concentrations of sCD25 were negatively associated with C-peptide concentrations (p = 4.8 × 10(-3)). CONCLUSIONS/INTERPRETATION: The 25% increase in sCD25 in patients, alongside the inverse association between sCD25 and C-peptide, probably reflect the adverse effects of an on-going, actively autoimmune and inflammatory immune system on beta cell function in patients.