In vivo distribution of β2 glycoprotein I under various pathophysiologic conditions

Agostinis, Chiara; Biffi, Stefania; Garrovo, Chiara; Durigutto, Paolo; Lorenzon, Andrea; Bek, Alpan; Bulla, Roberta; Grossi, Claudia; Borghi, Maria Orietta; Meroni, Pier Luigi; Tedesco, Francesco

doi:10.1182/blood-2011-01-333617

Cited by 113 publications

(120 citation statements)

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“…In addition, LPS or other bacterial PAMPs may induce the conformational change of β2GP1 into the fishhook-like structure, which facilitates the interaction of aPLA with β2GP1, thereby increasing their pathogenic effects. In case of pregnancy morbidity, instead of infection, hormonal changes could play a role in aPLA pathogenicity [61,62].…”

Section: The Role Of Members Of the Tlr Familymentioning

confidence: 99%

Receptors involved in cell activation by antiphospholipid antibodies

Brandt

Kruithof

Moerloose

2013

Thrombosis Research

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The antiphospholipid syndrome (APS) is an autoimmune disease associated with arterial or venous thrombosis and/or recurrent fetal loss and is caused by pathogenic antiphospholipid antibodies (aPLA). The plasma protein β2-glycoprotein 1 (β2GP1) has been identified as a major target of aPLA associated with APS. Cell activation by aPLA appears to be a major pathogenic cause in the pathogenesis of APS. Receptors, co-receptors and accessory molecules are known to assist the pathogenic effects of aPLA. Members of the TLR family and the platelet receptor apolipoprotein E receptor 2' (apoER2'), a receptor belonging to the low-density lipoprotein receptor (LDL-R) family, as well as GPIbα, were identified as putative candidates for aPLA recognition. CD14, a co-receptor for TLR2 and TLR4, and annexin A2, a ubiquitous Ca2+ -binding protein that is essential for actin-dependent vesicle transport, could serve as important accessory molecules in mediating the pathogenic effects of aPLA. Finally, complement activation has been reported in association with the pathogenicity of APS. The relative contribution of these different mechanisms in the pathogenesis of APS is controversial. Here, we review the various in vivo and in vitro models that have been used to investigate the pathogenic mechanisms of aPLA in APS

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Section: The Role Of Members Of the Tlr Familymentioning

confidence: 99%

Receptors involved in cell activation by antiphospholipid antibodies

Brandt

Kruithof

Moerloose

2013

Thrombosis Research

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“…8 The domain specificity of the anti-b2GPI scFv-Fc was investigated by ELISA using recombinant domains kindly provided by Dr P. G. De Groot (Amsterdam, The Netherlands). 22 To displace b2GPI-bound patient antibodies, immobilized human b2GPI (10 mg/mL) was first incubated with patient serum (1:200) for 30 minutes at room temperature and then with MBB2DCH2 (2 mg/100 mL) for an additional 30 minutes at room temperature.…”

Section: Antibody Binding Assaysmentioning

confidence: 99%

“…[4][5][6][7] We recently reported a significant increase in fetal loss in pregnant mice immunized with human b2GPI following the injection of a fluorescein-labeled purified protein that binds selectively to decidual endothelial cells and trophoblasts. 8 We also determined that the removal of anti-b2GPI antibodies from patient aPL-IgG using affinity chromatography significantly reduced the thrombotic effect in the rat mesenteric microcirculation. 9 Although aPL antibodies exhibit a modest reactivity with the soluble target molecules, it is widely accepted that the antibodies interact preferentially with b2GPI bound to endothelial cells, platelets, monocytes, and trophoblasts, all of which contribute to the pathogenesis of APS.…”

Section: Introductionmentioning

confidence: 99%

“…9,12 Although most of these observations were made using aPL of undefined specificity, the role of complement in inducing aPL-mediated blood clots and fetal resorption has been confirmed using specific antibodies to b2GPI. 8,9 In recent years, major efforts have been made to prevent aPLmediated thrombus formation and miscarriages. Currently, anticoagulants, such as heparin or warfarin, are used to prevent vascular thrombi, and a combination of low-dose aspirin and low-molecularweight heparin represents the first-line treatment of the obstetric complications of APS.…”

Section: Introductionmentioning

confidence: 99%

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A non–complement-fixing antibody to β2 glycoprotein I as a novel therapy for antiphospholipid syndrome

Agostinis

Durigutto

Sblattero

et al. 2014

Blood

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121

104

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Key Points• A recombinant antibody recognizing the D1 domain of b2 glycoprotein I induces fetal loss and clot formation in animal models.• The CH2-deleted antibody fails to activate complement and prevents the procoagulant and proabortive effects of patient antibodies.A single-chain fragment variable (scFv) recognizing b2-glycoprotein 1 (b2GPI) from humans and other species was isolated from a human phage display library and engineered to contain an IgG1 hinge-CH2-CH3 domain. The scFv-Fc directed against b2GPI domain I-induced thrombosis and fetal loss, thus mimicking the effect of antibodies from patients with antiphospholipid syndrome (APS). Complement is involved in the biological effect of anti-b2GPI scFv-Fc, as demonstrated by its ability to promote in vitro and in vivo complement deposition and the failure to induce vascular thrombosis in C6-deficient rats and fetal loss in C5-depleted mice. A critical role for complement was also supported by the inability of the CH2-deleted scFv-Fc to cause vessel occlusion and pregnancy failure. This antibody prevented the pathological effects of anti-b2GPI antibodies from APS patients and displaced b2GPI-bound patient antibodies. The CH2-deleted antibody represents an innovative approach potentially useful to treat APS patients refractory to standard therapy. (Blood. 2014;123(22):3478-3487)

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“…However, we still believe that obstetric APS does represent a distinct biological entity in comparison with the vascular variant. For example, β 2 -GPI is present only on the endothelial cells of uterine vessels but not on other vascular districts in resting animals; and aPL-positive IgG fractions from pure obstetric patients trigger different cell signaling in comparison with those from thrombotic APS sera 15,16 .…”

Section: Rheumatologymentioning

confidence: 99%