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Susceptibility for Lupus Nephritis by Low Copy Number of theFCGR3BGene Is Linked to Increased Levels of Pathogenic Autoantibodies
[摘要] Low copy number (CN) of theFCGR3Bgene reducesFCGR3Bmembrane expression on neutrophils and results in clearance of a smaller amount of immune complex. We investigatedFCGR3BCN in relation to the clinical phenotype in a Caucasian SLE cohort (n=107).FCGR3BCN was determined by three different qPCR parameter estimations (Ct−, Cy0, and cpD1) and confirmed by the FCGR2C/FCGR2A paralog ratio test. Clinical and serological data were then analyzed for their association withFCGR3BCN. LowFCGR3BCN (<2) was more frequent in SLE patients than in healthy controls (n=162) (20% versus 6%, OR 4.15,P=0.003) and associated with higher disease activity scores (SLEDAI 10.4 versus 6.1,P=0.03), lupus nephritis (LN) (25 versus 5%,P=0.03), and increased levels of antibodies against dsDNA (81 versus 37 IU,P=0.03), C1q (22 versus 6 IU,P=0.003), and ribosomal P (10 versus 5 IU,P=0.01). No such associations were seen with antibodies against extractable nuclear antigens or highFCGR3BCN (>2). In multivariate analyses, LN was independently associated with anti-C1q-Ab levels (P=0.03) and lowFCGR3BCN (P=0.09). We conclude that the susceptibility for LN in patients with lowFCGR3BCN is linked to increased levels of pathogenic autoantibodies.
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[效力级别]  [学科分类] 内科医学
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