HLA-DRB1 and MICA in Autoimmunity: Common Associated Alleles in Autoimmune Disorders

doi:10.1196/annals.1288.049

^aEndocrinology and Diabetes Research Group, Hospital de Cruces, Barakaldo, Basque Country, Spain
^bDepartment of Nursing, University of the Basque Country, Bilbao, Basque Country, Spain
^cPediatric Gastroenterology Unit, Hospital de Cruces, Barakaldo, Basque Country, Spain
^dDepartment of Pediatrics, University of the Basque Country, Bilbao, Basque Country, Spain

Autoimmune disorders such as type 1 diabetes (T1DM), celiacdisease (CD), and Addison's disease (ADD) develop in individualswith genetic susceptibility that are exposed to environmentaltriggering factors not completely defined. Patients with anautoimmune disease (and their relatives) are at increased riskof developing another disorder, and this might be caused bya common genetic origin of autoimmunity; for example, HLA classII region in 6p21 shows a very strong association with mostdiseases. The aim of this study was to determine whether sharedsusceptibility markers extend from the central (DRB1) throughthe telomeric (MICA) HLA region. We analyzed three independentsets of families with one autoimmune disease, T1DM, CD, or ADD,and genotyped them for HLA-DRB1 and for the exon 5 GCT polymorphismof MICA. For HLA-DRB1, allele DRB1*0301 was the only one associatedwith risk for all three diseases; in the case of MICA, alleleA9 was found to be the common protective allele. Haplotype analysisshows that haplotype A5.1-DRB1*0301 confers risk to autoimmunity.Our results show that there are common risk and protection allelesin both loci, suggesting a core of genetic association withautoimmunity (HLA-DRB1*0301 risk; A9 protection) that couldbe modulated by other alleles/loci or environmental factorstoward one or another disease. Some alleles are part of conservedhaplotypes (A5.1-DR3, A5.1-DR2), whereas others seem to haveindependent effect (A9) and support the idea of two independentloci in this region.

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