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C. Nalli, L. Andreoli, M. Motta, Z. Shums, M. Frassi, A. Lojacono, A. Meini, V. Medeghini, T. Avčin, A. Tincani
0 2011.

Lafinespecificitàdeglianticorpianti-b 2 glicoproteinaInellemalattieautoimmuni sistemicheèprevalentementediretta versoildominio1* Fine specificity of anti-b2glycoprotein I antibodies in systemic autoimmune diseases is mostly directed against domain 1

SUMMARY Objective: Anti-b 2 GPI are a formal laboratory criterion for the antiphospholipid syndrome (APS). They were demonstrated to be a risk factor for thrombosis and fetal losses but can also be detected in patients with systemic autoimmune disease (SAD), in healthy adults individuals and pre-school children. It has been suggested that different subpopulations of anti-b 2 GPI may carry different pathogenetic potential: autoantibodies against Domain1 seem to be associated with thrombosis; autoantibodies against Domain4/5 have been identifi ed in patients with non-thrombotic conditions. Methods: We studied 48 patients with SAD (32 systemic lupus erythematosus, 16 undifferentiated connettive tissue disease), 64 patients with APS, 57 one-year-old healthy children born to mother with SAD, 33 children with atopic dermatitis. All subjects were IgG anti-b 2 GPI positive. The specifiof anti-b 2 GPI was investigated using ELISA research products containing recombinant b 2 GPI D1 and D4/5 antigens. Cut-off values are calculated as 95th percentile on 100 NHD. IgG anti-b 2 GPI were tested at a validated home-made ELISA routinely performed in our laboratory. No thrombotic events were recordered in patients with SAD and in both groups of children. Results: Patients with SAD and APS showed prevalent reactivity for D1 while children in both groups preferentially recognize D4/5. Conclusions: IgG anti-b 2 GPI against D1 seem to cluster in patients with systemic autoimmune conditions. Their pathogenic potential in determine APS manifestations may be mitigated by adequate prophylaxis.


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