Abstract
The −863 C/A polymorphism in the tumor necrosis factor-α (TNF-α) promoter has been suggested to influence TNF-α expression. Here we elucidated the molecular mechanisms underlying the allele-specific regulation of TNF-α gene expression under basal and LPS-stimulated conditions in THP-1 cells and in human primary macrophages. We show that the binding of two NF-κB complexes, the p50/p50 homodimer and the p50/p65 heterodimer, was upregulated upon LPS stimulation. Both complexes bound to the C-allele whereas the A-allele only bound the p50/p65 complex. Two DNase I hypersensitive sites appeared in the TNF-α promoter after LPS stimulation of THP-1 cells. DNase I hypersensitivity of the TNF-α promoter was also analyzed in human monocytes prepared from individuals of different −863C/A genotype. Hypersensitivity was increased in the promoter harboring the mutant A-allele, particularly after LPS stimulation. In summary, binding of transcription factor NF-κB to the TNF-α promoter is associated with allele-specific remodeling of chromatin structure.
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