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C-antineutrophil cytoplasmic antibody positivity in vasculitis patients is associated with the Z allele of alpha-1-antitrypsin, and P-antineutrophil cytoplasmic antibody positivity with the S allele
Authors:Griffith, M. E.   Lovegrove, J. U.   Gaskin, G.   Whitehouse, D. B.   Pusey, C. D.
Affiliation:1Renal Unit, Royal Postgraduate Medical School, Hammersmith Hospital London, UK 2MRC Human Biochemical Genetics Unit, The Galton Laboratory, University College London London, UK
Abstract:BACKGROUND.: Antineutrophil cytoplasmic antibodies (ANCA) in vasculitis haveeither cANCA or pANCA patterns as defined by immunofluorescence.The target autoantigen of cANCA is usually proteinase 3 (PR3),whereas that of pANCA is usually myeloperoxidase (MPO). Alpha-1-antitrypsin({alpha}1AT) is the major physiological inhibitor of PR3, while MPOis an inhibitor of {alpha}1AT. METHODS.: To determine whether there was an association between ANCA positivevasculitis, ANCA pattern, and {alpha}1AT deficiency alleles, we studied{alpha}1AT phenotypes of 99 cANCA and 99 pANCA positive vasculitispatients by isoelectric focusing and immunoblotting, and comparedthem with 2310 controls from the same geographical area. RESULTS.: C-ANCA patients showed an increased frequency of the Z allele(0.055 versus 0.018 in controls), conferring a relative riskof 3. They showed no increase in frequency of the S allele.P-ANCA patients showed an increased frequency of the S allele(0.091 versus 0.046 in controls) conferring a relative riskof 2. The frequency of the Z allele also appeared to be increased(0.030 versus 0.018 in controls), but this was not statisticallysignificant. CONCLUSIONS.: These findings demonstrate an association between ANCA-positivevasculitis and deficiency phenotypes of {alpha}1AT, and suggest a rolefor {alpha}1AT in the development of systemic vasculitis.
Keywords:alpha-1-antitrypsin   ANCA   autoimmunity   myeloperoxidase   proteinase 3   systemic vasculitis   vasculitis
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