Prepregnancy

Idiopathic thrombocytopenic purpura is not a reason to discourage pregnancy; however, women with severe thrombocytopenia despite a splenectomy and high doses of corticosteroids are at high risk for complications and should have extensive preconception counselling about possible risks. When planning pregnancy, it is wise to optimise treatment before conception, mainly to assess the need for splenectomy before pregnancy.

Prenatal

Management of IPT during pregnancy requires a multidisciplinary approach, with a team including a haematologist, paediatrician (neonatologist), obstetrician and anaesthetist. A complete overview is displayed in Fig. 41.1 .

Recommendations for obstetric management in idiopathic thrombocytopenic purpura. CS, Caesarean section; IVIG, intravenous immunoglobulin.

During pregnancy, there are three indications for starting treatment: symptomatic women, a platelet count below 30 × 10 ⁹ /L or the need for a higher platelet count before a procedure (e.g., caesarean section).

When platelet counts are higher than 30 × 10 ⁹ /L, no treatment is necessary, and monitoring of maternal platelet counts needs to be performed every 2 weeks and more closely as delivery approaches.

First choice of treatment during pregnancy is similar to the approach in nonpregnant women, prednisone started at a dosage of 1 to 2 mg/kg/day and then tapered to find the minimal effective dose. If the thrombocytopenia shows to be resistant to corticosteroid treatment with prednisone or in case of serious side effects, intravenous infusion of immunoglobulins (IVIG) is next in line. Other treatments with limited evidence for their efficiency in ITP during pregnancy are intravenous anti-D infusion, splenectomy and azathioprine. Rituximab, danazol, Tpo receptor agonists and most other immunosuppressive drugs should not be administered during pregnancy because of possible teratogenicity. Platelet transfusions are only to be administered in very severe thrombocytopenia (platelet counts <20 × 10 ⁹ /L) and at times when there is a high risk for bleeding.

Labour and Delivery

Maternal platelet counts above 50 × 10 ⁹ /L are considered to be safe for vaginal as well as caesarean delivery. Therefore, if predelivery platelet counts are below 50 × 10 ⁹ /L, IVIG treatment should be administered at a dose of 0.8 kg/day. Although guidelines can differ among countries and centres, a platelet count above 80 × 10 ⁹ /L is considered safe for epidural analgesia. Treatment during pregnancy does not seem to have any effect on fetal platelet counts or the occurrence of neonatal bleeding problems; it should be administered for maternal indications only.

Initially, the management of labour and delivery in ITP patients was based on the concerns of ICH in the thrombocytopenic neonate, secondary to vaginal birth trauma. Therefore fetal scalp blood sampling or cordocentesis was performed, and caesarean delivery was preferred when fetal platelet count was below 50 × 10 ⁹ /L. Fetal scalp blood sampling appeared to yield falsely low counts, and predelivery cordocentesis, although producing reliable fetal platelet counts, has a significant risk for fetal loss and severe morbidity. In combination with the low incidence of perinatal bleeding, these should not be performed as routine procedures in patients with ITP. The route of delivery (vaginal or caesarean section) does not seem to affect the incidence of ICH; therefore, caesarean section in patients with ITP should only be performed for obstetric indications. Interventions such as fetal scalp blood sampling and vacuum extraction should be avoided during delivery.

Postnatal

An initial blood sample should be taken from the umbilical cord to assess the neonatal platelet count. Second, daily neonatal platelet counts should be done for approximately 1 week, depending on the presence and degree of neonatal thrombocytopenia detected. In addition, haemoglobin and bilirubin counts should be monitored. Cranial ultrasound is indicated only in case of severe thrombocytopenia. Postnatal treatment with IVIG is only indicated in case of severe neonatal thrombocytopenia (<50 × 10 ⁹ /L), and platelet transfusion should only be used in case of neonatal bleeding. Breastfeeding is not contraindicated.

Platelet Alloantigens and Alloantibodies

The platelet specific alloantigens, or HPAs, are carried by glycoprotein complexes that are present on the platelet membrane. Different HPA epitopes are created by single nucleotide polymorphisms (SNPs) that result in small changes in the glycoprotein structure through an amino acid change. Currently, there are 37 different types of HPAs described, located on six different glycoprotein complexes (IIb/IIIa, Ib/IX, Ia/IIa and CD109) on the platelet membrane.

For a recent overview, see http://www.ebi.ac.uk/ipd/hpa/table1.html . The 12 most frequently involved HPAs are clustered into six biallelic groups ( Table 41.2 ). The greater portion of all HPA are localised on glycoprotein (GP) IIb/GP IIIa, also called integrin αIIbβ3, the fibrinogen receptor, which is the most abundant molecule on the surface of platelets. GP IIb contains 7 and GP IIA 16 different HPA systems. Although all HPAs that are present on GP IIIa can be involved in FNAIT, HPA-1a is the predominant cause of FNAIT, especially in the Caucasian population. HPA-1a accounts for approximately 80% of cases followed by HPA-5b, responsible for about 10% of cases of FNAIT ( Table 41.3 ). In the Asian population, however, anti–HPA-4b is the most frequently involved alloantibody followed by anti–HPA-3a and anti–HPA-21b. Furthermore, alloantibodies against GP IV/CD36 seem to have an increased presence in the African and Asian populations.

The immune response to alloantigens is mediated by human leukocyte antigen (HLA) class II molecules. Antigen-presenting cells such as dendritic cells, macrophages and B lymphocytes process the antigens into small peptides, which are presented by the HLA class II antigens on their surfaces. CD4-positive T-helper lymphocytes can recognise the peptide–HLA complex, leading to the activation of the T cell. Activated T cells then interact with B lymphocytes, initiating antibody production. After active transport, through FcRn, of the formed alloantibodies against the fetal antigens enter the fetal circulation and induce destruction of fetal platelets.

The GP that carries the most important alloantigen in FNAIT, HPA-1a, is GP IIIa, which is also called ‘integrin β3’. On platelets, integrin β3 is complexed to GP IIb. In addition to this complex, integrin β3 can form a complex with αV as well. This αVβ3 complex, still carrying the HPA-1a epitope, is scarcely expressed on platelets but is prominently present on the surface of endothelial cells, vascular smooth muscle cells and syncytiotrophoblast cells. The presence of HPA-1a on these different cell types, other than platelets, and interaction of maternal alloantibodies with these cells might reveal new mechanisms in the pathophysiology.

Vascular Integrity

The exact pathogenic mechanism leading to devastating ICH in FNAIT has never been adequately understood. Generally, alloantibodies were thought to enter the fetal circulation and cause bleeding problems through destruction of fetal platelets resulting in thrombocytopenia. However, only a small proportion of the severely thrombocytopenic newborns have a severe haemorrhage, indicating another mechanism to be involved. Because integrin β3 that carries the HPA-1a epitope is also present on endothelial cells (in complex with αV; αVβ3), it has been suggested that interaction of anti–HPA-1a with endothelial cells plays a key role in the development of bleeding complications. In vitro studies already illuminated the direct interaction between anti–HPA-1a and human umbilical vein endothelial cells (HUVECs), demonstrated by a decreased HUVEC spreading as well as a decreased integrity of their monolayer in electric cell–substrate impedance sensing (ECIS) assays. In addition, in vivo animal studies showed that mice without circulating platelets and or fibrinogen do not show any bleeding problems in utero . This supports the hypothesis that instead of the thrombocytopenia and blood coagulation, another mechanism plays a key role in causing bleeding complications. Recently, a large study with both active and passive murine models of anti–HPA-1a mediated FNAIT has been performed and showed that ICHs in these mice occurred regardless of platelet count. Also, HPA-1a antibodies inhibited angiogenic signalling, induced endothelial cell apoptosis and decreased vessel density in affected brains as well as retinas. This delivered the first direct evidence for αVβ3 integrin’s role in angiogenesis and HPA-1a–induced impaired angiogenesis in mice, suggesting this to be a key factor in causing bleeding complications in FNAIT. The first analysis with a small number of human sera containing HPA-1a antibodies concluded that the interaction of the antibodies with endothelial cells might determine and possibly predict the occurrence of ICH.

Placental Function

In addition to platelets and endothelial cells, integrin β3 is also expressed on placental tissue by syncytiotrophoblast cells in αVβ3 complex as well. Although there is no direct evidence, it has been suggested that anti–HPA-1a might induce placental insufficiency through interaction with these syncytiotrophoblast cells, demonstrated by a strong association with intrauterine growth restriction, as well as cases of intrauterine fetal demise (in absence of bleeding problems). In addition, in a group of 13 FNAIT cases, lymphoplasmacytic chronic villitis was found to be significantly more present in placenta tissue of untreated cases when compared to cases treated with IVIG. Another correlation that has been suggested is one between FNAIT and miscarriages. In addition, the expression of HPA-1a on placental tissue might lead to increased and early exposure to the fetal HPA-1a and might be a possible explanation for FNAIT already affecting first pregnancies and first-born children in FNAIT.

Overall, there is increasing evidence of more advanced pathophysiologic mechanisms initiated by anti-HPA-1a, than solely platelet destruction.

Human Leukocyte Antigen

Specific HLA class II molecules seem to be associated with the occurrence of alloimmunisation in HPA incompatible pregnancies. HLA-DRB3∗0101 was found to be positively correlated to the occurrence HPA-1a alloimmunisation in HPA-1a–negative pregnant women. The underlying mechanism suggested is the difference in the ability to form stable bonds between Pro33/Leu33, the amino acids present on the integrin β3 peptides of HPA-1b alleles and HPA-1a alleles, respectively.

There is some evidence that HLA class I plays a role in FNAIT as well. In contrast to HLA class II molecules, HLA class I molecules are expressed on platelet membranes. With an expression of approximately 20,000 HLA class I molecules, platelets are the major source of HLA class I present in blood. Maternal alloimmunisation against fetal HLA on platelets, possibly causing antibody-mediated fetal thrombocytopenia in a similar mechanism to HPA alloantibodies is mentioned in a number of case reports. In contrast to what previously has been thought, HLA class I alloantibodies can cross the placental barrier and do enter the fetal circulation. Whether or not these antibodies can actually be held responsible for fetal and neonatal thrombocytopenia is not clear yet. Strong evidence to support such a causal relationship is currently lacking.