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Please use this identifier to cite or link to this item: http://hdl.handle.net/20.500.12710/19166
Title: The Lupus Anticoagulant paradox
Authors: Prichici, Victoria
Cimpoi, Aurelia
Keywords: lupus anticoagulant;prothrombin;thrombosis
Issue Date: 2021
Publisher: Universitatea de Stat de Medicină şi Farmacie "Nicolae Testemiţanu" din Republica Moldova
Citation: PRICHICI, Victoria, CIMPOI, Aurelia. The Lupus Anticoagulant paradox: [poster]. In: Conferinţa ştiinţifică anuală "Cercetarea în biomedicină și sănătate: calitate, excelență și performanță", 20-22 octombrie 2021: culegere de postere. 2021, p. 25.
Abstract: Introduction: Purpose: The goal of the research is to present the reasons that cause the respective prolongation of the coagulation time induced by LA to be mostly associated with thrombosis, than with a tendency to bleed. Material and methods: For the research was studied the specialty literature on biochemical perspectives and mechanisms of The lupus anticoagulant paradox. Results: Conclusions: Lupus anticoagulants are a heterogeneous class of immunoglobulins (predominantly IgG autoantibodies and, rarely, IgM), which bind specifically to the epitopes of negatively charged plasma phospholipid binding proteins, prothrombin, beta2-glycoprotein I (most commonly, domain D I of the molecule is involved) or annexin V, inhibiting phospholipid-dependent coagulation in vitro. LA forms an APLA subgroup that disrupts the in vitro assembly of the prothrombinase complex (factors Xa, Va and prothrombin in the complex on phospholipid membranes), leading to prolongation of aPTT, diluted Russell viper venom time (dRVVT), coagulation time kaolin plasma and rarely prothrombin time. In vivo, the mechanism of thrombosis is explained by Ig G binding to phospholipids, a phenomenon that is essential for the degradation of the normal effects of protein C and protein S, thus changing the balance in favor of thrombus formation. There are many mechanisms for inducing LA, including infections, oxidative stress, and major stress, such as surgery or trauma. All of these stressors help expose phospholipids, which eventually allow antibodies to attach. At this turn, this leads to intravascular coagulation and thrombus formation. Lupus anticoagulant has procoagulant properties in vivo and prolongs coagulation times addicted to phospholipid in vitro. Extended in vitro coagulation time may be mistaken as a bleeding disorder. Different thromboplastin reagents and plasma mixing assays, as well as independent thromboplastin coagulation assays may be useful to differentiate in vitro changes associated with LA from in vivo coagulation factor deficiency. Laboratory Diagnosis of the Lupus Anticoagulant β2GPI and antibody. β2GPI and antibody to β2GPI binding to a phospholipid surface. B2GPI consists of 5 homologous domains. Domain V binds to the anionic phospholipid surface. The antiβ2GPI antibody binds to domain I. The prevalence of thrombosis in patients with lupus anticoagulants is 24-36%; deep limb thrombosis and pulmonary embolism predominate. Patients with recurrent miscarriages have lupus anticoagulants in approximately 10% of cases. The prevalence of LA in patients with SLE is attested only in 5-10% of cases. Conclusions: Lupus anticoagulant has procoagulant properties in vivo and prolongs coagulation times addicted to phospholipid in vitro. Extended in vitro coagulation time may be mistaken as a bleeding disorder. Different thromboplastin reagents and plasma mixing assays, as well as independent thromboplastin coagulation assays may be useful to differentiate in vitro changes associated with LA from in vivo coagulation factor deficiency.
metadata.dc.relation.ispartof: Conferinţa ştiinţifică anuală "Cercetarea în biomedicină și sănătate: calitate, excelență și performanță", 20-22 octombrie 2021
URI: http://repository.usmf.md/handle/20.500.12710/19166
Appears in Collections:Conferinţa ştiinţifică anuală "Cercetarea în biomedicină și sănătate: calitate, excelență și performanță", 20-22 octombrie 2021: Culegere de postere

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