Human Molecular Genetics, Vol 6, 1011-1016, Copyright © 1997 by Oxford University Press
P Reed, F Cucca, S Jenkins, M Merriman, A Wilson, P McKinney, E Bosi, G Joner, K Ronningen, E Thorsby, D Undlien, T Merriman, A Barnett, S Bain and J Todd
A region of linkage to type 1 diabetes has been defined on human chromosome
10p11-q11 (IDDM10; P = 0.0007) using 236 UK and 76 US affected sibpairs and
a 1 cM resolution microsatellite marker map. Analysis by the transmission
disequilibrium test (TDT) in 1159 families with at least one diabetic
child, from the UK, the US, Norway, Sardinia and Italy provided additional
support for linkage at D10S193 (P = 0.006, Pc = 0.17). Notably, 5.1 cM
distal to D10S193, marker D10S588 also provided positive TDT results (P =
0.009, Pc = 0.25) but the allele under analysis was also preferentially
transmitted to nonaffected siblings (P = 0.0008, Pc = 0.02). This allele
was positively associated in an independent UK case control study and,
importantly, was neutrally transmitted in control CEPH families. These
results suggest a type 1 diabetes susceptibility locus on chromosome
10p11-q11 (provisionally designated IDDM10) and demonstrate the necessity
of analysis of non affected siblings in disease families, as well as
analysis of control families.
ARTICLES
Evidence for a type 1 diabetes susceptibility locus (IDDM10) on human chromosome 10p11-q11
The Wellcome Trust Centre for Human Genetics, Nuffield Department of Surgery, University of Oxford, UK.
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