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The International Psoriasis Genetics Study: Assessing Linkage to 14 Candidate Susceptibility Loci in a Cohort of 942 Affected Sib Pairs

Authors :
R Mistry
Stefan Jenisch
Jwn Barker
James T. Elder
Colin Veal
Alan Menter
Nicholas V.C. Chia
Mark J. Daly
A D Burden
Enno Christophers
Philip E. Stuart
Tilo Henseler
D Tillman
Cynthia Helms
Francesca Capon
Rajan P. Nair
John J. Voorhees
M Allen
Anne M. Bowcock
Richard C. Trembath
Source :
The American Journal of Human Genetics. 73:430-437
Publication Year :
2003
Publisher :
Elsevier BV, 2003.

Abstract

In an effort to confirm previously reported linkages to psoriasis, we analyzed 942 affected sibling pairs (ASPs) from 710 pedigrees for 53 polymorphic microsatellites spanning 14 psoriasis candidate regions at an intermarker spacing of approximately 5 cM. Maximum LOD score (MLS) analysis of ASPs yielded allele sharing of 60% for markers within the major histocompatibility complex (MHC) (P=2 x 10(-14)), which yielded a gene-specific lambda(s) of 1.6. Across the remainder of the genome, the strongest evidence of allele sharing was obtained on chromosomes 16q (D16S3032; MLS=1.3; P=.007) and 10q22-q23 (D10S2327; MLS=1.1; P=.012). None of the remaining loci exceeded MLS=0.9, the value expected to occur by chance once in this study. In agreement with previous studies, strong linkage disequilibrium was also observed between psoriasis and the MHC (pedigree disequilibrium test P=3.9 x 10(-8) for D6S1014). Two psoriasis-associated MHC haplotypes were identified with the haplotype-based transmission/disequilibrium test. Analysis of only those families carrying either of these haplotypes significantly increased the chromosome 16q LOD score from 1.3 to 2.4 (P=.045). These results underscore the importance of the MHC in psoriasis and provide a rationale for more-detailed examination of candidate regions on chromosomes 16q and 10q.

Details

ISSN :
00029297
Volume :
73
Database :
OpenAIRE
Journal :
The American Journal of Human Genetics
Accession number :
edsair.doi.dedup.....d884ec189dbe53848dbaba75f6bb5818
Full Text :
https://doi.org/10.1086/377159