RT Journal Article
SR Electronic
T1 Apolipoprotein H Promoter Polymorphisms in Relation to Lupus and Lupus-related Phenotypes
JF The Journal of Rheumatology
JO J Rheumatol
FD The Journal of Rheumatology
SP 315
OP 322
DO 10.3899/jrheum.080482
VO 36
IS 2
A1 SANGITA SURESH
A1 F. YESIM K. DEMIRCI
A1 ERIN JACOBS
A1 AMY H. KAO
A1 ELISA Y. RHEW
A1 DHARAMBIR K. SANGHERA
A1 FAITH SELZER
A1 KIM SUTTON-TYRRELL
A1 DAVID McPHERSON
A1 FRANKLIN A. BONTEMPO
A1 CANDACE M. KAMMERER
A1 ROSALIND RAMSEY-GOLDMAN
A1 SUSAN MANZI
A1 M. ILYAS KAMBOH
YR 2009
UL http://www.jrheum.org/content/36/2/315.abstract
AB Objective. Sequence variation in gene promoters is often associated with disease risk. We tested the hypothesis that common promoter variation in the APOH gene (encoding for ß2-glycoprotein I) is associated with systemic lupus erythematosus (SLE) risk and SLE-related clinical phenotypes in a Caucasian cohort. Methods. We used a case-control design and genotyped 345 women with SLE and 454 healthy control women for 8 APOH promoter single-nucleotide polymorphisms (SNP; –1284C&gt;G, –1219G&gt;A, –1190G&gt;C, –759A&gt;G, –700C&gt;A, –643T&gt;C, –38G&gt;A, and –32C&gt;A).Association analyses were performed on single SNP and haplotypes. Haplotype analyses were performed using EH (Estimate Haplotype–frequencies) and Haploview programs. In vitro reporter gene assay was performed in COS-1 cells. Electrophoretic mobility shift assay (EMSA) was performed using HepG2 nuclear cells. Results. Overall haplotype distribution of the APOH promoter SNP was significantly different between cases and controls (p = 0.009). The –643C allele was found to be protective against carotid plaque formation (adjusted OR 0.37, p = 0.013) among patients with SLE. The –643C allele was associated with a ~2-fold decrease in promoter activity as compared to wild-type –643T allele (mean ± standard deviation: 3.94 ± 0.05 vs 6.99 ± 0.68, p = 0.016). EMSA showed that the –643T&gt;C SNP harbors a binding site for a nuclear factor. The –1219G&gt;A SNP showed a significant association with the risk of lupus nephritis (age-adjusted OR 0.36, p = 0.016). Conclusion. Our data indicate that APOH promoter variants may be involved in the etiology of SLE, especially the risk for autoimmune-mediated cardiovascular disease.