Contribution of MHC class I chain-related A (MICA) gene polymorphism to genetic susceptibility for systemic lupus erythematosus

doi:10.1093/rheumatology/keh459

Rheumatology Advance Access originally published online on November 2, 2004
Rheumatology 2005 44(3):287-292; doi:10.1093/rheumatology/keh459

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Contribution of MHC class I chain-related A (MICA) gene polymorphism to genetic susceptibility for systemic lupus erythematosus

G. Gambelunghe¹^,5, R. Gerli², E. Bartoloni Bocci², P. Del Sindaco⁴, M. Ghaderi⁶, C. B. Sanjeevi⁵, O. Bistoni², V. Bini³ and A. Falorni¹

¹ Department of Internal Medicine, Section of Internal Medicine and Endocrine and Metabolic Sciences, ² Center for the Study of Rheumatic Diseases, Department of Clinical and Experimental Medicine and ³ Department of Gynaecology, Obstetrics and Paediatric Sciences, University of Perugia, Perugia, ⁴ Division of Medicine, Todi Hospital, Todi, Italy, ⁵ Department of Molecular Medicine, Karolinska Institute, Stockholm and ⁶ Division of Biomedicine, Institution for Healthcare Sciences, Örebro University, Örebro, Sweden.

Correspondence to: A. Falorni, Department of Internal Medicine, Section of Internal Medicine and Endocrine and Metabolic Sciences, Via E. Dal Pozzo, 06126 Perugia, Italy. E-mail: falorni{at}dimisem.med.unipg.it

Objective. To evaluate the contribution of the MHC class I chain-relatedA (MICA) gene polymorphism to the genetic risk of systemic lupuserythematosus (SLE).

Methods. HLA-DRB1-DQA1-DQB1 genotyping, MICA exon 5 microsatellitegenotyping and HLA-B8 genotyping were performed in 48 ItalianSLE patients and in 158 healthy control subjects.

Results. Of HLA class II haplotypes, only DRB1*03-DQA1*0501-DQB1*0201(DR3-DQ2) was significantly more frequent among SLE patientsthan among healthy control subjects [odds ratio (OR) = 6.5,corrected P<0.0026]. HLA-B8 was detected in 31% SLE patientsand 13% healthy control subjects (OR = 3.0, P = 0.005). Theallele-wise comparison between patients and controls showedthat both MICA5 (OR = 2.5, corrected P<0.0005) and MICA5.1(OR = 2.4, corrected P<0.0005) were positively and MICA9(OR = 0.2, corrected P<0.0005) was negatively associatedwith the disease. The MICA5/5.1 genotype was positively associatedwith SLE (OR = 28.9, corrected P<0.0015) also in subjectsnegative for DR3-DQ2 (OR>22.6, corrected P<0.011). Thesimultaneous presence of DR3-DQ2 and MICA5.1 was detected in15/48 (31%) SLE and in 10/158 (6%) healthy control subjects(OR = 6.7, corrected P<0.011). The simultaneous combinationof DR3-DQ2 and MICA5 was found in 10/48 (21%) SLE patients andin only 1/158 healthy control subjects (OR = 41.3, correctedP<0.011). Logistic regression analysis showed the independentpositive associations of MICA5 and MICA5.1 and negative associationof MICA9 with the disease, and revealed that the interactionof the three major markers (DR3-DQ2, MICA5 and MICA5.1) wasassociated with increasing genetic risk, which was highest (OR>30.3)in DR3-DQ2-positive subjects carrying the MICA5-5.1 genotype.

Conclusions. Our study provides the first demonstration of theindependent association of the MICA gene polymorphism with geneticrisk of SLE.

KEY WORDS: Autoimmunity, Immunogenetics, HLA, MICA gene, systemic lupus erythematosus

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