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3 research outputs found

Common variants in WFS1 confer risk of type 2 diabetes

Author: A Karasik
AC Riggs
AL Gloyn
Allan Daly
Andrew D Morris
Andrew T Hattersley
Benjamin Glaser
Charlotte Kimber
Colin N A Palmer
D Altshuler
EM Nielsen
Graham Hitman
H Inoue
H Ishihara
Hana Lango
Ilana Blech
Inês Barroso
JA Minton
Jon Wasson
K Silander
Katherine A Fawcett
LD Love-Gregory
M Alan Permutt
Manjinder S Sandhu
Mark I McCarthy
Mark Walker
Michael N Weedon
Nicholas J Wareham
Paul D Pharoah
Richard Sherva
Roger Tavendale
Rosalind J Neumann
Sally L Debenham
SF Grant
T Yamada
Timothy M Frayling
TM Strom
U Ozcan
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2007
Field of study

We studied genes involved in pancreatic beta cell function and survival, identifying associations between SNPs in WFS1 and diabetes risk in UK populations that we replicated in an Ashkenazi population and in additional UK studies. In a pooled analysis comprising 9,533 cases and 11,389 controls, SNPs in WFS1 were strongly associated with diabetes risk. Rare mutations in WFS1 cause Wolfram syndrome; using a gene-centric approach, we show that variation in WFS1 also predisposes to common type 2 diabetes

Crossref

PubMed Central

Edinburgh Research Explorer

Oxford University Research Archive

University of Dundee Online Publications

Genomic sequence of the class II region of the canine MHC: Comparison with the MHC of other mammalian species

Author: Ashurst Jennifer L.
Binns Matthew M.
Debenham Sally L.
Hart Elizabeth A.
Howe Kevin L.
Ollier William E R
Quail Michael A.
Publication venue: 'Elsevier BV'
Publication date: 01/01/2005
Field of study

The University of Manchester - Institutional Repository

Bayesian Meta-Analysis of Genetic Association Studies with Different Sets of Markers

Author: Benjamin Emelia J.
Boekholdt Matthijs S.
Casas Juan P.
Cavalleri Gianpiero
Chapman Juliet
Debenham Sally L.
Hingorani Aroon D.
Humphries Steve E.
Judson Richard
Kathiresan Sekar
Khaw Kay Tee
Larson Martin G.
Rong Jian
Sandhu Manjinder
Shah Tina
Smeeth Liam
Sofat Reecha
Verzilli Claudio
Wareham Nicholas J.
Whittaker John C.
Publication venue: American Society of Human Genetics
Publication date: 01/01/2008
Field of study

Robust assessment of genetic effects on quantitative traits or complex-disease risk requires synthesis of evidence from multiple studies. Frequently, studies have genotyped partially overlapping sets of SNPs within a gene or region of interest, hampering attempts to combine all the available data. By using the example of C-reactive protein (CRP) as a quantitative trait, we show how linkage disequilibrium in and around its gene facilitates use of Bayesian hierarchical models to integrate informative data from all available genetic association studies of this trait, irrespective of the SNP typed. A variable selection scheme, followed by contextualization of SNPs exhibiting independent associations within the haplotype structure of the gene, enhanced our ability to infer likely causal variants in this region with population-scale data. This strategy, based on data from a literature based systematic review and substantial new genotyping, facilitated the most comprehensive evaluation to date of the role of variants governing CRP levels, providing important information on the minimal subset of SNPs necessary for comprehensive evaluation of the likely causal relevance of elevated CRP levels for coronary-heart-disease risk by Mendelian randomization. The same method could be applied to evidence synthesis of other quantitative traits, whenever the typed SNPs vary among studies, and to assist fine mapping of causal variants

Elsevier - Publisher Connector

LSHTM Research Online

PubMed Central

UCL Discovery