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Genes in the HLA class I region may contribute to the HLA class II-associated genetic susceptibility to multiple sclerosis
Authors:Harbo H F  Lie B A  Sawcer S  Celius E G  Dai K-Z  Oturai A  Hillert J  Lorentzen A R  Laaksonen M  Myhr K-M  Ryder L P  Fredrikson S  Nyland H  Sørensen P S  Sandberg-Wollheim M  Andersen O  Svejgaard A  Edland A  Mellgren S I  Compston A  Vartdal F  Spurkland A
Institution:Institute of Immunology, Rikshospitalet University Hospital, Oslo, Norway.
Abstract:In order to analyze whether loci in the human leukocyte antigen (HLA) class I region may contribute to the HLA class II-associated genetic susceptibility to multiple sclerosis (MS), we examined selected microsatellite markers in 177 Nordic sib-pair families, 222 British sib-pair families, 323 sporadic Norwegian MS patients and 386 Norwegian controls. All samples were, in addition, genotyped for the HLA-DR DQ haplotype, and the Norwegian case-control samples were also typed for HLA-A and -B loci. In the Norwegian sporadic MS patients association was seen with HLA-A, HLA-B, and with the D6S265 marker, located 100 kb centromeric to HLA-A. Associations with HLA-A and D6S265 loci were also suggested when restricting the analysis to HLA-DR15 haplotypes. In the sib-pair data a similar trend was seen with marker D6S265. Higher genotypic relative risk (GRR) was found for individuals who carry both HLA-DR15 and -A3 (GRR = 15), compared to those who carry only HLA-DR15 (GRR = 7), only HLA-A3 (GRR = 3) or none of these alleles (GRR = 1). The highest risk was conferred by a combination of HLA-DR15 and -A3 (odds ratio (OR) = 5.2). These results suggest that HLA-A or a gene in linkage disequilibrium with it may contribute to the HLA class II-associated genetic susceptibility to MS.
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