Myasthenia gravis and tumor necrosis factor beta polymorphisms: linkage disequilibrium but no association beyond HLA-B8.

Abstract	Tumor necrosis factor (TNF) may contribute to the susceptibility for autoimmune diseases. We examined TNFbeta gene polymorphisms detected by AspHI and NcoI digestion of genomic DNA in patients with myasthenia gravis (n=105) and healthy controls (n=114). In both groups, the frequencies of TNFbeta alleles were not different. AspHI and NcoI polymorphisms of TNFbeta showed a strong association with HLA-B8 (p < 0.03 resp. p < 0.0001 for AspHI and Ncol) both in patients and controls. Our results imply linkage disequilibrium of TNFbeta alleles with HLA-B8 and in myasthenia gravis we were unable to show a stronger association beyond HLA-B8.
Authors	M G Manz, A Melms, N Sommer, C A Müller
Journal	Journal of neuroimmunology (J Neuroimmunol) Vol. 90 Issue 2 Pg. 187-91 (Oct 01 1998) ISSN: 0165-5728 [Print] Netherlands
PMID	9817446 (Publication Type: Journal Article)
Chemical References	HLA-B8 Antigen HLA-DR Antigens Lymphotoxin-alpha
Topics	Adult Aged Alleles Female HLA-B8 Antigen (genetics) HLA-DR Antigens (genetics) Humans Linkage Disequilibrium Lymphotoxin-alpha (genetics) Male Middle Aged Myasthenia Gravis (genetics)

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