Learning Objectives
Review the association between inherited thrombophilia and recurrent miscarriage
Discuss key evidence informing anticoagulation use and pregnancy outcomes in women with inherited thrombophilia and recurrent miscarriage
CLINICAL CASE
A 32-year-old woman was referred to you at 15 weeks gestation regarding anticoagulation management. She has a history of 2 prior miscarriages at weeks 12 and 15, and she reports that she has a homozygous prothrombin gene mutation (PGM). She denies any personal or family history of venous thromboembolism. How would you approach anticoagulation in this patient?
Introduction
Recurrent pregnancy loss (RPL) affects 1%-5% of couples, placing a significant psychological and physical burden on women and families and increasing health care costs. The etiology for RPL remains unexplained in half of the cases despite extensive evaluation, and physicians and patients resort to treatment modalities that have uncertain benefit in an attempt to achieve a healthy live birth. Inherited thrombophilia (IT) has been associated with increased risk of venous thromboembolism (VTE) during pregnancy and the postpartum period. The association of IT with placenta-mediated pregnancy complications, including pregnancy loss, small-for-gestational-age fetus, preeclampsia, and placental abruption, has remained controversial for several years due to discordant results from various studies.1,2 In this review, we summarize key studies examining the association between IT and RPL and studies examining the role of anticoagulation in preventing pregnancy loss in women with IT and a history of miscarriage. VTE prevention and outcomes in acquired thrombophilias, such as antiphospholipid antibody syndrome, are outside the scope of this review.
Inherited thrombophilia and pregnancy outcomes
Common ITs include factor V Leiden (FVL) and prothrombin G20210A (PGM) mutations, and deficiency of natural anticoagulants, protein C, protein S and antithrombin III. The risk of VTE during pregnancy in these disorders varies widely depending on the underlying mutation (odds ratio [OR] of 3.19 for protein S deficiency, to 34.4 for women with homozygous FVL mutation compared to those without IT) (Table 1). Their associations with pregnancy-related outcomes showed lower absolute risks.2 The European Prospective Cohort on Thrombophilia study showed increased risk of still birth or late fetal loss with thrombophilia, although the likelihood of a positive outcome is high in both women with thrombophilia and in controls, with no clear benefit of anticoagulation.3 A meta-analysis of 10 prospective studies showed a weak association between FVL and late pregnancy loss.4 A recent meta-analysis of 89 studies involving 30 254 individuals demonstrated an association of RPL with FVL and PGM mutations (homozygous or heterozygous) in first and second trimesters and an association of protein S deficiency with late term fetal loss, but no association of RPL with antithrombin or protein C deficiency. The majority of the studies included in this meta-analysis did not control for confounders and included very few patients with high-risk thrombophilia, such as homozygous FVL and PGM (Table 2).5 These studies were plagued by heterogeneity in study population, outcomes, and small sample sizes and demonstrated low absolute risk for RPL in IT or no clear association between the two conditions, leading to the American College of Obstetricians and Gynecologists (ACOG) guidelines recommending against routine testing for IT in women with RPL.6
Prevalence and impact of inherited thrombophilia on pregnancy associated thrombosis or recurrent pregnancy loss
| Thrombophilia | Prevalence in the general population (%)8 | Venous thromboembolism risk in pregnancy (OR, 95% CI)3 | Risk of recurrent pregnancy loss (OR, 95% CI)6 |
|---|---|---|---|
| Homozygous factor V Leiden | <1% | 34.4 (9.86-120.05) | 2.76 (1.34-5.71) |
| Heterozygous factor V Leiden | 3.7% | 8.32 (5.44-12.70) | 2.07 (1.57-2.72) |
| Homozygous PGM | <1% | 26.36 (1.24-559.29) | 2.33 (0.87-6.26) |
| Heterozygous PGM | 0.7%-4% | 6.8 (2.46-18.77) | 1.69 (1.17-2.45) |
| Antithrombin deficiency | 0.02% | 4.69 (1.30-16.96) | 0.83 (0.29-2.36) |
| Protein C deficiency | 0.2% | 4.76 (2.15-10.57) | 1.98 (0.97-4.04) |
| Protein S deficiency | 0.03%-0.13% | 3.19 (1.48-6.88) | 3.45 (1.15-10.35) |
| Thrombophilia | Prevalence in the general population (%)8 | Venous thromboembolism risk in pregnancy (OR, 95% CI)3 | Risk of recurrent pregnancy loss (OR, 95% CI)6 |
|---|---|---|---|
| Homozygous factor V Leiden | <1% | 34.4 (9.86-120.05) | 2.76 (1.34-5.71) |
| Heterozygous factor V Leiden | 3.7% | 8.32 (5.44-12.70) | 2.07 (1.57-2.72) |
| Homozygous PGM | <1% | 26.36 (1.24-559.29) | 2.33 (0.87-6.26) |
| Heterozygous PGM | 0.7%-4% | 6.8 (2.46-18.77) | 1.69 (1.17-2.45) |
| Antithrombin deficiency | 0.02% | 4.69 (1.30-16.96) | 0.83 (0.29-2.36) |
| Protein C deficiency | 0.2% | 4.76 (2.15-10.57) | 1.98 (0.97-4.04) |
| Protein S deficiency | 0.03%-0.13% | 3.19 (1.48-6.88) | 3.45 (1.15-10.35) |
Selected studies examining the impact of anticoagulation on pregnancy outcomes in women with inherited thrombophilia
| Author, year, sample size | Inclusion criteria | Inherited thrombophilia Sample Size | Intervention | Live birth outcome* | Overall findings for impact of anticoagulation on live birth | |
|---|---|---|---|---|---|---|
| All inherited thrombophilias N (%) | Sample size of FVL or PGM homozygosity (N) | |||||
| Randomized controlled trials | ||||||
| Quenby, 2023 N = 326 | Women with FVL, PGM, AT, PC or PS, and RPL | 326 (100%) | N = 5 FVL HOM N = 5 in Group 1 N = 0 in Group 2 N = 2 PGM HOM N = 0 in Group 1, N = 2 in Group 2 | Group 1: LMWH Group 2: no treatment | 72% Group 1 71% Group 2 | No difference on live birth outcomes |
| Karadag, 2020 N = 174 | Women with FVL and RPL | 174 (100%) | 62 = FVL HOM N = 23 in Group 1, N = 21 in Group 2, N = 18 in Group 3 | Group 1: Aspirin Group 2: LMWH + ASA Group 3: LMWH | 86.9% Group 1 86.4% Group 2 83.3% Group 3 | No difference on live birth outcomes |
| Schleussner, 2015 N = 449 | Women with a history of at least 2 consecutive early miscarriages or 1 late miscarriage Patients were then screened for FVL, PGM, AT, PS, PC | 63 (14%) | FVL HOM and PGM HOM patients were excluded | Group 1: LMWH Group 2: No treatment | 86% Group 1 86.7% Group 2 | No difference on live birth outcomes |
| Rodger, 2014 N = 289 | Women with FVL, PGM, AT, PS, PC or APS and previous pregnancy complications or venous thromboembolism risk factors 62/164 in intervention group and 67/143 in control group had history of pregnancy loss | 283 (97%) | N = 4 FVL HOM Did not specify which group | Group 1: LMWH Group 2: No treatment | Pregnancy Loss Group 1: 8.2% Group 2: 7% | No difference on pregnancy loss outcomes |
| Martinelli, 2012 N = 135 | Women with FVL, PGM, AT, PS, PC and history of pregnancy complications (25/67 in intervention and 24/68 in control group had a history of intrauterine fetal death) | 131 (97%) | Did not specify | Group 1: LMWH Group 2: No treatment | Intrauterine fetal death Group 1: 3.2% Group 2: 1.5% | No difference in intrauterine fetal death |
| Visser, 2011 N = 207 | Women with RPL, with or without FVL, PGM, PS, PC | 26 (12.5%) | Specifically excluded high risk thrombophilia of FVL HOM or PGM HOM | Group 1: LMWH + placebo Group 2: LMWH + ASA Group 3: ASA | Group 1: 71% Group 2: 65% Group 3: 61% Outcomes in IT: Group 1: 13/17 Group 2: 9/15 Group 3: 12/19 | No difference on pregnancy loss outcomes |
| Clark, 2010 N = 294 | Women with at least 2 consecutive early pregnancy losses, once enrolled each was screened for IT | 10 (3%) | None | Group 1: LMWH + ASA Group 2: No treatment | Pregnancy loss Group 1: 22% Group 2: 20% | No difference on pregnancy loss outcomes |
| Kaandorp, 2010 N = 364 | Women with FVL, PGM, AT, PS, PC and a history of unexplained recurrent miscarriages | 47 (12%) | Did not specify | Group 1: LMWH + ASA Group 2:ASA Group 3: Placebo | Group 1: 69.1% Group 2: 61.6% Group 3: 67% | No difference in live birth rate |
| Laskin, 2009 N = 88 | Women with FVL, PGM, PS, PC, MTHFR mutation, positive antinuclear antibody, or positive antiphospholipid antibody and a history of recurrent pregnancy loss | 19 (21.5%) | None | Group 1: LMWH + ASA Group 2: ASA | Group 1: 77.8% Group 2: 79.1% | No difference on pregnancy loss outcomes |
| Gris, 2004 N = 160 | Women with FVL, PGM, PS, and 1 unexplained pregnancy loss | 160 (100%) | None | Group 1: LMWH Group 2: ASA | Group 1: 86% Group 2: 29% | The only RCT that showed a benefit to LMWH |
| Observational Studies | ||||||
| Dugalic, 2019 Prospective N = 358 | Women with (FVL, PGM, AT, PC, PS; also included PA1, and MTHFR) with previous pregnancy outcomes including miscarriage and intrauterine fetal demise | 195 (54%) | Did not specify | Group 1: LMWH Group 2: Control | Group 1: 100% Group 2: 91.5% | Live birth rate was higher when LMWH was implemented |
| Calvijo, 2019 Retrospective N = 88 | Women with IT (FVL, PGM, AT, PC, PS) Early pregnancy loss <10 weeks (26/88) Late pregnancy loss >10 weeks (11/88) | 88 (100%) | None | Group 1: before IT diagnosis, and no LMWH Group 2: following IT, treated with LMWH | OR for miscarriage (M) or fetal loss (FL) following LMWH use: M: 0.41 (0.20-0.82) P = 0.012 FL: 0.08 (00.5-1.39) P = 0.085 | Miscarriage rate was lower when LMWH was implemented |
| Aracic, 2016 Prospective N = 50 | Women with IT and history of adverse pregnancy outcomes (conventional IT: FVL, PGM, AT, PC, PS) and others included (MTHFR, PAI-1 polymorphism, ACE polymorphism) 80/128 prior pregnancies resulted in first or second term pregnancy loss | 50 (100%) | None | Group 1: LMWH Group 2 = no treatment | Group 1: 96% Group 2: 37.5% | Live birth rate was higher when LMWH was implemented |
| Aynioglu, 2016 Retrospective N = 153 | Women with history of prior pregnancy loss and IT (FVL, PGM, AT, PS, PC and included MTHFR) | 153 (100%) | N = 1 FVL HOM Group 1 N = 1 PGM HOM Group 2 | Group 1: LMWH + ASA Group 2: untreated | Proportion of the 85 live births in the cohort attributed to each group: Group 1: 80% Group 2: 20% | Live birth rate was higher in intervention group |
| Sokol, 2016 Retrospective N = 70 | Women with IT (FVL, PGM, AT, PS, PC, and MTHFR) with mean number of prior pregnancy loss >1 | 70 (100%) | N = 1 FVL HOM N = 1 PGM HOM | Group 1: LMWH Group 2: control | Miscarriage rate Group 1: 1.7% Group 2: 30% | Miscarriage rate was lower when LMWH was implemented |
| Tormene, 2012 Bidirectional N = 416 | Women with FVL or PGM Mean number of prior pregnancy loss Group 1: 1.15 Group 2: 1.58 Group 3: 1.52 Group 4: 0.53 | 416 (100%) | Group 1: N = 1 PGM HOM N = 8 FVL HOM N = 14 compound heterozygotes Group 2: none Group 3: none Group 4: N = 2 PGM HOM, N = 14 FVL HOM, N = 23 compound heterozygotes | Group 1: LMWH Group 2: LMWH + ASA Group 3: ASA Group 4: none | LMWH protective effect on miscarriages (OR 0.52; 95% CI, 0.29-0.94) | Miscarriage rate was lower when LMWH was implemented |
| Kupferminc, 2011 Retrospective N = 116 | Women with IT (FVL, PGM, PS, PC) and history of adverse pregnancy outcomes 17/87 in Group 1 had pregnancy loss 6/29 in Group 2 had pregnancy loss | 116 (100%) | Did not specify | Group 1: LMWH Group 2: no treatment | Pregnancy loss >20 weeks Group 1: 0 Group 2: 7% | LMWH did not change pregnancy loss >20 weeks |
| Grandone, 2008 Retrospective N = 32 | Women with pregnancy loss and AT, PS or PS | 32 (100%) | Did not specify | Group 1: LMWH in 8 pregnancies Group 2: no treatment in 95 pregnancies | Group 1: 88.9% Group 2: 28.4% | Live birth rate was higher with LMWH |
| Carp, 2003 Prospective N = 85 | Women with IT (FVL, PGM, AT, PS, PC, and MTHFR) and pregnancy loss | 85 (100%) | Did not specify | Group 1: LMWH Group 2: no treatment | Group 1: 70.2% Group 2: 43.8% | Live birth rate was higher with LMWH |
| Brenner, 2000 Prospective N = 50 | Women with IT (FVL, PGM, PS, PC, MTHFR), also included APS and recurrent pregnancy loss | 50 (100%) | Did not specify | Group 1: LMWH Group 2: no treatment | Group 1:75% Group 2: 20% | Live birth rate was higher with LMWH |
| Author, year, sample size | Inclusion criteria | Inherited thrombophilia Sample Size | Intervention | Live birth outcome* | Overall findings for impact of anticoagulation on live birth | |
|---|---|---|---|---|---|---|
| All inherited thrombophilias N (%) | Sample size of FVL or PGM homozygosity (N) | |||||
| Randomized controlled trials | ||||||
| Quenby, 2023 N = 326 | Women with FVL, PGM, AT, PC or PS, and RPL | 326 (100%) | N = 5 FVL HOM N = 5 in Group 1 N = 0 in Group 2 N = 2 PGM HOM N = 0 in Group 1, N = 2 in Group 2 | Group 1: LMWH Group 2: no treatment | 72% Group 1 71% Group 2 | No difference on live birth outcomes |
| Karadag, 2020 N = 174 | Women with FVL and RPL | 174 (100%) | 62 = FVL HOM N = 23 in Group 1, N = 21 in Group 2, N = 18 in Group 3 | Group 1: Aspirin Group 2: LMWH + ASA Group 3: LMWH | 86.9% Group 1 86.4% Group 2 83.3% Group 3 | No difference on live birth outcomes |
| Schleussner, 2015 N = 449 | Women with a history of at least 2 consecutive early miscarriages or 1 late miscarriage Patients were then screened for FVL, PGM, AT, PS, PC | 63 (14%) | FVL HOM and PGM HOM patients were excluded | Group 1: LMWH Group 2: No treatment | 86% Group 1 86.7% Group 2 | No difference on live birth outcomes |
| Rodger, 2014 N = 289 | Women with FVL, PGM, AT, PS, PC or APS and previous pregnancy complications or venous thromboembolism risk factors 62/164 in intervention group and 67/143 in control group had history of pregnancy loss | 283 (97%) | N = 4 FVL HOM Did not specify which group | Group 1: LMWH Group 2: No treatment | Pregnancy Loss Group 1: 8.2% Group 2: 7% | No difference on pregnancy loss outcomes |
| Martinelli, 2012 N = 135 | Women with FVL, PGM, AT, PS, PC and history of pregnancy complications (25/67 in intervention and 24/68 in control group had a history of intrauterine fetal death) | 131 (97%) | Did not specify | Group 1: LMWH Group 2: No treatment | Intrauterine fetal death Group 1: 3.2% Group 2: 1.5% | No difference in intrauterine fetal death |
| Visser, 2011 N = 207 | Women with RPL, with or without FVL, PGM, PS, PC | 26 (12.5%) | Specifically excluded high risk thrombophilia of FVL HOM or PGM HOM | Group 1: LMWH + placebo Group 2: LMWH + ASA Group 3: ASA | Group 1: 71% Group 2: 65% Group 3: 61% Outcomes in IT: Group 1: 13/17 Group 2: 9/15 Group 3: 12/19 | No difference on pregnancy loss outcomes |
| Clark, 2010 N = 294 | Women with at least 2 consecutive early pregnancy losses, once enrolled each was screened for IT | 10 (3%) | None | Group 1: LMWH + ASA Group 2: No treatment | Pregnancy loss Group 1: 22% Group 2: 20% | No difference on pregnancy loss outcomes |
| Kaandorp, 2010 N = 364 | Women with FVL, PGM, AT, PS, PC and a history of unexplained recurrent miscarriages | 47 (12%) | Did not specify | Group 1: LMWH + ASA Group 2:ASA Group 3: Placebo | Group 1: 69.1% Group 2: 61.6% Group 3: 67% | No difference in live birth rate |
| Laskin, 2009 N = 88 | Women with FVL, PGM, PS, PC, MTHFR mutation, positive antinuclear antibody, or positive antiphospholipid antibody and a history of recurrent pregnancy loss | 19 (21.5%) | None | Group 1: LMWH + ASA Group 2: ASA | Group 1: 77.8% Group 2: 79.1% | No difference on pregnancy loss outcomes |
| Gris, 2004 N = 160 | Women with FVL, PGM, PS, and 1 unexplained pregnancy loss | 160 (100%) | None | Group 1: LMWH Group 2: ASA | Group 1: 86% Group 2: 29% | The only RCT that showed a benefit to LMWH |
| Observational Studies | ||||||
| Dugalic, 2019 Prospective N = 358 | Women with (FVL, PGM, AT, PC, PS; also included PA1, and MTHFR) with previous pregnancy outcomes including miscarriage and intrauterine fetal demise | 195 (54%) | Did not specify | Group 1: LMWH Group 2: Control | Group 1: 100% Group 2: 91.5% | Live birth rate was higher when LMWH was implemented |
| Calvijo, 2019 Retrospective N = 88 | Women with IT (FVL, PGM, AT, PC, PS) Early pregnancy loss <10 weeks (26/88) Late pregnancy loss >10 weeks (11/88) | 88 (100%) | None | Group 1: before IT diagnosis, and no LMWH Group 2: following IT, treated with LMWH | OR for miscarriage (M) or fetal loss (FL) following LMWH use: M: 0.41 (0.20-0.82) P = 0.012 FL: 0.08 (00.5-1.39) P = 0.085 | Miscarriage rate was lower when LMWH was implemented |
| Aracic, 2016 Prospective N = 50 | Women with IT and history of adverse pregnancy outcomes (conventional IT: FVL, PGM, AT, PC, PS) and others included (MTHFR, PAI-1 polymorphism, ACE polymorphism) 80/128 prior pregnancies resulted in first or second term pregnancy loss | 50 (100%) | None | Group 1: LMWH Group 2 = no treatment | Group 1: 96% Group 2: 37.5% | Live birth rate was higher when LMWH was implemented |
| Aynioglu, 2016 Retrospective N = 153 | Women with history of prior pregnancy loss and IT (FVL, PGM, AT, PS, PC and included MTHFR) | 153 (100%) | N = 1 FVL HOM Group 1 N = 1 PGM HOM Group 2 | Group 1: LMWH + ASA Group 2: untreated | Proportion of the 85 live births in the cohort attributed to each group: Group 1: 80% Group 2: 20% | Live birth rate was higher in intervention group |
| Sokol, 2016 Retrospective N = 70 | Women with IT (FVL, PGM, AT, PS, PC, and MTHFR) with mean number of prior pregnancy loss >1 | 70 (100%) | N = 1 FVL HOM N = 1 PGM HOM | Group 1: LMWH Group 2: control | Miscarriage rate Group 1: 1.7% Group 2: 30% | Miscarriage rate was lower when LMWH was implemented |
| Tormene, 2012 Bidirectional N = 416 | Women with FVL or PGM Mean number of prior pregnancy loss Group 1: 1.15 Group 2: 1.58 Group 3: 1.52 Group 4: 0.53 | 416 (100%) | Group 1: N = 1 PGM HOM N = 8 FVL HOM N = 14 compound heterozygotes Group 2: none Group 3: none Group 4: N = 2 PGM HOM, N = 14 FVL HOM, N = 23 compound heterozygotes | Group 1: LMWH Group 2: LMWH + ASA Group 3: ASA Group 4: none | LMWH protective effect on miscarriages (OR 0.52; 95% CI, 0.29-0.94) | Miscarriage rate was lower when LMWH was implemented |
| Kupferminc, 2011 Retrospective N = 116 | Women with IT (FVL, PGM, PS, PC) and history of adverse pregnancy outcomes 17/87 in Group 1 had pregnancy loss 6/29 in Group 2 had pregnancy loss | 116 (100%) | Did not specify | Group 1: LMWH Group 2: no treatment | Pregnancy loss >20 weeks Group 1: 0 Group 2: 7% | LMWH did not change pregnancy loss >20 weeks |
| Grandone, 2008 Retrospective N = 32 | Women with pregnancy loss and AT, PS or PS | 32 (100%) | Did not specify | Group 1: LMWH in 8 pregnancies Group 2: no treatment in 95 pregnancies | Group 1: 88.9% Group 2: 28.4% | Live birth rate was higher with LMWH |
| Carp, 2003 Prospective N = 85 | Women with IT (FVL, PGM, AT, PS, PC, and MTHFR) and pregnancy loss | 85 (100%) | Did not specify | Group 1: LMWH Group 2: no treatment | Group 1: 70.2% Group 2: 43.8% | Live birth rate was higher with LMWH |
| Brenner, 2000 Prospective N = 50 | Women with IT (FVL, PGM, PS, PC, MTHFR), also included APS and recurrent pregnancy loss | 50 (100%) | Did not specify | Group 1: LMWH Group 2: no treatment | Group 1:75% Group 2: 20% | Live birth rate was higher with LMWH |
(or similar) for entire population (not just IT group).
ACE, angiotensin converting enzyme polymorphism; APS, antiphospholipid antibody syndrome; ASA, aspirin; AT, antithrombin deficiency; HOM, homozygosity; PC, protein C deficiency; PS, protein S deficiency.
Anticoagulation and pregnancy outcomes in inherited thrombophilia
The pathophysiology of adverse pregnancy outcomes in thrombophilia is multifactorial, and thrombosis of placental vasculature is unlikely to be the sole mechanism.7 While guidelines exist for thromboprophylaxis during pregnancy and the postpartum setting in women with IT,6,8,9 some physicians have adopted low-molecular-weight heparin (LMWH) for management of women with IT and RPL due to presumed benefit of anticoagulation, extrapolating from studies in patients with antiphospholipid antibody syndrome. A review of the literature identified 10 randomized controlled studies (RCTs) and 10 observational studies (Table 2) evaluating the effect of anticoagulation on live birth rates in women with IT and a history of pregnancy loss.
A prospective cohort study including 126 women with a thrombophilia and history of pregnancy loss showed increased live births with LMWH (OR 10.6; 95% CI, 5.0-22.3), concluding that LMWH was beneficial in preventing pregnancy loss.10 However, there was no reduction in adverse pregnancy outcomes with LMWH compared with placebo in the Thrombophilia in Pregnancy Prophylaxis trial (risk difference, -1.8%; 95% CI, -10.6% to 7.1% in intention-to-treat analysis), with increased risk of minor bleeding with LMWH.11 A Cochrane review of aspirin, LMWH, or both in women with RPL showed no difference in live birth rates or other obstetric complications when these treatments were compared to a placebo.12 A meta-analysis of observational studies suggested improved live birth rate,13 but a meta-analysis of 8 RCTs in IT and pregnancy loss did not show a significant difference in live birth rate with the use of LMWH compared with no LMWH (relative risk [RR] 0.81; 95% CI: 0.55-1.19).14 The recently completed randomized controlled ALIFE2 study enrolled 326 women with IT and ≥2 pregnancy losses and showed no difference in live birth rates or other adverse pregnancy outcomes with LMWH compared to standard of care (OR, 1.08; 95% CI, 0.65 to 1.78; absolute risk difference: 0.7%), supporting that there is no benefit of anticoagulation to improve live birth rate.
Does type of thrombophilia matter?
The discrepancy in findings from observational studies and RCTs emphasizes the heterogeneity and confounding factors in interpretation of these studies. Most of these studies included White individuals and patients with low-risk thrombophilia; some included participants with nonconventional ITs, such as a methylenetetrahydrofolate reductase (MTHFR) mutation or a plasminogen activator inhibitor-1 (PAI-1) polymorphism (Table 2). These studies highlight the lack of evidence specifically in high-risk thrombophilias, which are managed distinctly within guidelines for VTE risk reduction in pregnancy even in women with no personal or family history.8 This also provides an opportunity to conduct further studies in diverse populations with high-risk thrombophilia. It is extremely challenging to recruit patients in these clinical trials, as seen with ALIFE2 study, which took several years to recruit patients despite multinational collaboration, but we can agree upon the recommendations against routine antepartum LMWH prophylaxis in women with heterozygous FVL or PGM mutations.15
Risks with anticoagulation
Anticoagulant use in pregnancy, as in any situation, must be weighed against the risk of complications related to bleeding. A Cochrane review of aspirin or anticoagulant use in women with RPL demonstrated no increased risk of bleeding with aspirin alone, but an increased risk when LMWH was used in combination with aspirin (RR, 2.28; 95% CI, 1.6-3.24).12 The ALIFE2 study revealed no difference in bleeding between women treated with LMWH vs placebo, though 45% of women treated with LMWH experienced bruising compared to 10% of control participants.16 In addition to bleeding, anticoagulation during pregnancy is inconvenient, increases the risk of osteopenia, adds to health care costs, and gives false hope to women.
Conclusions
Empiric anticoagulation during pregnancy in women with IT and RPL has not been confirmed to confer any benefit regarding pregnancy outcomes other than thromboembolism prevention in high risk women.
Screening for IT is not recommended for women with RPL, as there is insufficient evidence that antepartum thromboprophylaxis improves the live birth rate (conditional recommendation, very low certainty in evidence about effects).
Patients with IT and RPL do not benefit from prophylactic LMWH, as it has not been shown to increase live birth rate, and we do not recommend routine use of anticoagulation to improve pregnancy outcomes in these individuals (conditional recommendation, very low certainty in evidence about effects).
RCTs have repeatedly demonstrated no benefit of antepartum anticoagulation to improve live birth rate in women with IT and RPL and provide reassurance to women with thrombophilia. The ACOG guidelines recommend low dose aspirin for women at high risk of preeclampsia but not specifically for RPL.17 In our patient with homozygous PGM and RPL, antepartum anticoagulation is not likely to increase the chance of a live birth. The American Society of Hematology guidelines suggest against antepartum anticoagulation in the absence of a family history of thrombosis, but postpartum thromboprophylaxis is recommended to prevent a first VTE.9
Future directions
There is insufficient evidence to recommend anticoagulation as an intervention to prevent adverse pregnancy outcomes in women with IT. Future research delineating the role of placental pathology and subgroups of women with a thrombophilia that might benefit from anticoagulation would be helpful.
Acknowledgments
Radhika Gangaraju received funding from the National Heart, Lung, and Blood Institute (K08 HL159290) and the American Society of Hematology and research support from Sanofi.
Conflict-of-interest disclosure
Leslie Padrnos: no competing financial interests to declare.
Radhika Gangaraju served as a consultant for Sanofi, Bayer, Takeda and Alexion.
Off-label drug use
Leslie Padrnos: Nothing to disclose.
Radhika Gangaraju: Nothing to disclose.
