PREGNANCY
THROMBOPROPHYLAXIS
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Acquired thrombophilia (antiphospholipid syndrome) |
Am J Obstet
Gynecol. 2000 Oct;183(4):1008-12.
Does aspirin have a role in improving pregnancy outcome for women with the
antiphospholipid syndrome? A randomized controlled trial.
Pattison NS, Chamley LW, Birdsall M, Zanderigo AM, Liddell HS, McDougall J.
Department of Obstetrics and Gynaecology, University of Auckland, Auckland,
New Zealand.
Objectives:
This pilot investigation was undertaken to assess the efficacy of
low-dose aspirin therapy for the treatment of women with antiphospholipid
antibodies when recurrent miscarriage is the only sequela. Study Design:
A
double-blind, randomized, placebo-controlled trial was conducted in the
setting of the recurrent miscarriage clinic of a tertiary referral obstetric
hospital. The participants were 50 women with a history of recurrent
miscarriages (>/=3) and antiphospholipid antibodies. Women with systemic
lupus erythematosus or a history of thrombosis were excluded. Women were
recruited after full investigative screening at the recurrent miscarriage
clinic. Women with >/=3 fetal losses and persistently positive results for
antiphospholipid antibodies were randomly allocated to receive either
aspirin (75 mg daily) or placebo. Investigators, clinicians, and patients
were blinded to the treatment. Rates of live births, antenatal
complications, and delivery and neonatal outcomes were recorded
prospectively. Data were compared by chi(2) analysis with Yates' correction,
the Fisher exact test, or the Student t test as appropriate. Results:
There
were 10 exclusions after random assignment because of inappropriate
inclusion. Eighty-five percent of the placebo (17/20) group and 80% of the
aspirin-treated group (16/20) were delivered of live infants. This
difference was not significant. There were no significant differences in
antenatal complications or neonatal morbidity between the groups.
Conclusions:
This preliminary study suggests that low-dose aspirin has no
additional benefit when added to supportive care for women for whom
recurrent early fetal loss is the only sequela of the antiphospholipid
syndrome. This live birth rate with supportive care alone exceeds the
published live birth rates for women with antiphospholipid antibody-mediated
recurrent fetal loss who were treated with heparin or corticosteroids. This
trial, like all other trials in this field, is small, but its results bring
into question the need for pharmacologic intervention for women with
antiphospholipid syndrome for whom recurrent fetal loss is the only sequela.
Our results highlight the need for a large randomized controlled trial to
identify the optimal treatment for this group of women and justify the
inclusion of a placebo arm in any such trial.

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