Objective
The objective of the study was to investigate whether resistance to annexin A5 anticoagulant activity (AnxA5) occurs in women with histories for obstetric complications of antiphospholipid syndrome (Obs-APS) and whether this correlates with antibody recognition of domain 1 of β2-glycoprotein.
Study Design
One hundred thirty-six women with antiphospholipid antibodies, including 70 with histories for Obs-APS and 30 controls, were investigated.
Results
Women with Obs-APS showed resistance to AnxA5 activity (median, 216%; range, 130–282% vs controls; median, 247%; range, 217–283%; P < .0001) and elevated levels of anti-domain I immunoglobulin (Ig) G (optical density: median, 0.056; range, 0.021–0.489 vs median, 0.042; range, 0.020–0.323; P = .002). Those in the lowest tertile of AnxA5 anticoagulant ratios had an odds ratio for Obs-APS of 58.0 (95% confidence interval, 3.3–1021.5). There was an inverse correlation between levels of annexin A5 anticoagulant activity and anti-domain I IgG.
Conclusion
Resistance to AnxA5 anticoagulant activity is associated with antibody recognition of domain I of β2-glycoprotein I and identifies a subset of women with histories for Obs-APS.
The antiphospholipid syndrome (APS) is defined by the association of a persistently abnormal antiphospholipid antibody (aPL) assays (ie, elevated immunoassays anticardiolipin and/or anti-β2glycoprotein I immunoglobulin (Ig) G or IgM antibodies or a positive lupus anticoagulant test) with a history of thrombosis or specific pregnancy complications.
The currently available antiphospholipid assays are empirically derived tests that do not measure a disease mechanism; the immunoassays were derived from the biological false-positive syphilis phenomenon and the lupus anticoagulant from the observation an inhibitor to the activated partial thromboplastin time, both described more than 50 years ago. The pathogenic mechanism for obstetric APS has remained enigmatic.
The syndrome is referred to as primary APS (PAPS) when it occurs without other autoimmune disease and secondary APS when it is associated with another autoimmune disease, usually systemic lupus erythematosus. In this paper, the term obstetric APS applies to aPL associated with the pregnancy complications that were defined by consensus diagnostic criteria; these include a previous unexplained recurrent first trimester loss and/or midtrimester and third-trimester intrauterine death and/or severe preeclampsia, placental abruption, or intrauterine growth retardation.
The purpose of this study was to investigate whether women with histories of obstetric APS might have evidence for resistance to annexin A5 (AnxA5) anticoagulant activity in their blood. AnxA5 is a placental anticoagulant protein that is highly expressed on the apical surfaces of syncytiotrophoblasts in which the protein is in an anatomic position to play a thrombomodulatory role and contribute to the fluidity of the maternal circulation through the intervillous space.
The protein is also expressed in a number of other cell types including, among others, vascular endothelial cells, renal tubular epithelial cells, and bile duct epithelial cells. The protein’s potent anticoagulant activities result from its forming 2-dimensional crystals over anionic phospholipids that shield the phospholipids from contributing to critical phospholipid-dependent coagulation enzyme reactions. The aPL antibodies have been shown to reduce the quantity of AnxA5 on cultured placental trophoblasts and accelerate the coagulation of plasma that is exposed to these cells . Furthermore, aPL antibodies reduce the binding of AnxA5 to phospholipid bilayers and create significant defects in the ordered crystallization of this protein that expose unshielded phospholipids, thereby accelerating coagulation enzyme reactions.
We previously reported that patients with APS-associated vascular thrombosis had resistance to AnxA5 anticoagulant activity and that this reduced AnxA5 anticoagulant activity correlated strongly with antibody-mediated displacement of AnxA5 from binding to phospholipids and with antibody recognition of a specific epitope on domain 1 of β 2 -glycoprotein I (β2GPI).
We also previously reported that women with a history of recurrent spontaneous pregnancy losses, not screened for aPL antibodies, had reduced AnxA5 anticoagulant activity. However, the specific question of whether there may be evidence for resistance to annexin A5 anticoagulant activity in the blood of women with aPL-associated pregnancy complications has never been previously investigated. Nor has the question of whether anti-domain 1 IgG antibodies might correlate with obstetric APS been previously investigated.
Therefore, the aim of this study was to measure these specific parameters in women with histories of obstetric APS. Because of the inflammatory state induced by systemic lupus erythematosus, the study was confined to patients with PAPS.
Materials and Methods
Patients
After obtaining local ethical committee approval at Guy’s and St Thomas’s Trust, blood specimens were collected with informed consent from healthy, nonpregnant women who had a history of obstetric PAPS and both men and women with a diagnosis of thrombotic PAPS or isolated aPL antibodies. All PAPS patients satisfied the Miyakis criteria for the diagnosis of aPL and APS.
In total, 136 patients with aPL antibodies were classified into 3 groups: (1) women, not currently pregnant but with a past history of obstetric PAPS (n = 70); (2) subjects without obstetric APS but with a history of thrombotic PAPS, with their last thrombotic event more than 6 months previously (n = 50); and (3) subjects with isolated aPL antibodies who had not sustained any thrombotic or pregnancy events (n = 16).
The demographic, aPL characteristics including types of obstetric APS and treatment details are summarized in Table 1 . There was no significant difference in ages between groups, but obviously, those with obstetric PAPS were all female, and the majority of the other groups were also female. As described in Table 1 , 29 of the 70 women with obstetric APS had histories for 3 or more spontaneous first-trimester losses, 39 of the women had a history for intrauterine fetal demise, and 26 had histories for placental insufficiency.
| Demographic | Group A, obstetric APS | Group B, thrombotic APS | Group C, aPL only | Group D, healthy controls |
|---|---|---|---|---|
| Number | 70 | 50 | 19 | 30 |
| Age, y, median (range) | 40 (25–58) | 41 (20–64) | 38 (22–68) | |
| Female:male | 70:0 | 39:11 | 15:4 | 30:0 |
| aPL status | ||||
| Thrombotic history | 23 (30%) | 50 (100%) | 0 | 0 |
| Arterial only | 8 (11%) | 20 (40%) | ||
| Venous only | 9 (13%) | 21 (42%) | ||
| Venous and arterial | 6 (8%) | 9 (18%) | ||
| Previous pregnancy morbidity | ||||
| Recorded first-trimester loss a | 15 | |||
| Death of fetus >10/40 b | 18 | |||
| Placental insufficiency c | 15 | |||
| Both a and b | 11 | |||
| Both b and c | 8 | |||
| Both a and c | 1 | |||
| a and b and c | 2 | |||
| Antithrombotic medication | ||||
| Aspirin | 32 (46%) | 6 (12%) | 9 (47%) | |
| Warfarin | 27 (39%) | 40 (80%) | 0 | |
| LMWH | 0 | 1 (2%) | 0 | |
| Nil | 11 (16%) | 8 (16%) | 10 (53) | |
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