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Target Concepts:
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Query: UNIPROT:P02749 (
beta2-glycoprotein I
)
836
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The mechanism of thrombosis in patients with antiphospholipid syndrome is not clear. To investigate it, we examined the effect of monoclonal anticardiolipin (aCL) antibodies and
beta2-glycoprotein I
(
beta2-GPI
), which is required for formation of the aCL epitopes, on activated protein C (APC) and on fibrinolytic activity. First, APC activities were measured in the presence and absence of
beta2-GPI
or gamma M immunoglobulin (IgM) monoclonal aCLs (EY1C8 and EY2C9), or both, established from peripheral blood lymphocytes obtained from a patient with aCL.
beta2-GPI
exhibited a procoagulant activity by inhibiting APC activity as well as an anticoagulant activity by inhibiting thrombin generation. Any further inhibition of APC activity was caused by monoclonal aCL, and then only in the presence of
beta2-GPI
. The remaining tissue plasminogen activator (t-PA) of the sample consisting of
beta2-GPI
, two-chain recombinant
t-PA
, and plasminogen activator inhibitor (PAI)-1 was measured by a chromogenic assay using the synthetic substrate S-2251, Glu-plasminogen, and soluble fibrin monomer.
beta2-GPI
protected
t-PA
activity from inhibition by PAI-1. However, monoclonal aCLs (EY1C8 and EY2C9) inhibited the effect of
beta2-GPI
on fibrinolytic activity; that is, monoclonal aCLs inhibited fibrinolytic activity by elevating PAI-1 activity. Thrombosis in patients with aCL can be explained in part by both the inhibition of APC anticoagulant activity and the impairment of fibrinolytic activity by aCL.
...
PMID:The putative mechanism of thrombosis in antiphospholipid syndrome: impairment of the protein C and the fibrinolytic systems by monoclonal anticardiolipin antibodies. 1062 10
The fifth domain (DV) of
beta2-glycoprotein I
(beta2GPI) is important for binding a number of ligands including phospholipids and factor XI (FXI). Beta2GPI is proteolytically cleaved in DV by plasmin but not by thrombin, VIIa,
tissue plasminogen activator
, or uPA. Following proteolytic cleavage of DV by plasmin, beta2GPI retains binding to FXI but not to phospholipids. Native beta2GPI, but not cleaved beta2GPI, inhibits activation of FXI by thrombin and factor XIIa, attenuating a positive feedback mechanism for additional thrombin generation. In this report, we have defined the FXI/FXIa binding site on beta2GPI using site-directed mutagenesis. We show that the positively charged residues Lys284, Lys286, and Lys287 in DV are essential for the interaction of beta2GPI with FXI/FXIa. We also demonstrate that FXIa proteolytically cleaves beta2GPI at Lys317-Thr318 in DV. Thus, FXIa cleavage of beta2GPI in vivo during thrombus formation may accelerate FXI activation by decreasing the inhibitory effect of beta2GPI.
...
PMID:Domain V of beta2-glycoprotein I binds factor XI/XIa and is cleaved at Lys317-Thr318. 1552 84
Thrombocytopenia prevalance and its association with antiphospholipid syndrome, disorders of the hemostasis system, the course and activity of the disease have been studied in SLE patients. 10.5% of 457 SLE patients in central and western part of Ukraine had thrombocytopenia which non-significantly depended on sex, age and disease duration but was tightly associated with cardiovascular disorders. Thrombocytopenia appears as an independent risk factor for vascular disorders which does not depend on lipid metabolic disorders and system inflammatory reaction but is firmly associated with the presence of antiphospholipid syndrome,
beta-2-glycoprotein I
levels, thrombocyte hyperactivity, antithrombin III and
tissue plasminogen activator
deficiency.
...
PMID:[Thrombocytopenia in patients with systemic lupus erythematosis as a risk factor for thrombotic complications and its connection with severity and the course of the disease, systemic lupus erythematosis]. 1871 94
