Abstract
Objective
To establish linkage and replicate the association of macrophage migration inhibitory factor (MIF) with juvenile idiopathic arthritis (JIA).
Methods
Three hundred twentyโone Caucasian simplex families from the UK were genotyped for polymorphisms of MIF using SNaPshot ddNTP primer extension, or by a fluorescently labeled primer method, and capillary gel electrophoresis. The functional significance of the promoter polymorphisms was studied using luciferaseโbased reporter gene assays in human T lymphoblast and epithelial cell lines.
Results
MIF was linked and associated with JIA (P = 0.0016). Specifically, a 2โpoint promoter haplotype, CATT~7~โMIFโ173*C, was found to be transmitted in excess (38 transmitted: 21 not transmitted) in the JIA patients. Conditional extended transmission disequilibrium test and pairwise extended transmission disequilibrium test predicted functional interaction between the 2 polymorphic positions. The interaction of the CATT repeat with MIFโ173*G/C was found to be specific to the cell type.
Conclusion
Replication of an association and linkage of MIF with JIA has been established. Functional interaction between the polymorphic positions on the linked haplotype has also been shown. The molecular mechanism of this interaction is currently being investigated.