Fetal anaemia and related disorders

Question 1

At what two points in pregnancy should women have their blood group and antibody status determined?

Answer 1

Booking
28/40

Collect 28/40 sample before Anti-D administration

Question 2

If Rh -, at what gestations in pregnancy should women be offered Anti-D, and why?

Answer 2

28/40 and 34/40
625IU
To prevent iso-immunisation

Due to the risk of spontaneous sensitisation that can occur at this gestation

Question 3

If Rh-, what care should women receive postnatally?

Answer 3

Dose of Anti-D (routine prophylaxis, 625IU) within 72 hours

Measurement of Kleihauer: quantification of fetal-maternal haemorrhage

Question 4

What proportion of women are Rh negative

Answer 4

1 in 7

Question 5

What proportion of women will have
- red cell antibodies
- clinically significant antibodies
detected in pregnancy?

Answer 5

Red cell antibodies = 1.2%

Clinically significant antibodies = 0.4%

Question 6

What are 5 examples of sensitising events in the first trimester, that would be indications for Anti-D in a Rh negative woman

Answer 6

Miscarriage
MTOP or STOP
Ectopic pregnancy
CVS

There is insufficient evidence to suggest that a threatened miscarriage before 12/40 necssitates Anti-D (RANZCOG)
NZ Blood Bank advises to give Anti-D due to a small risk of anti-D isoimmunisation

250IU unless multiple pregnancy: 625IU

Question 7

What are 5 examples of sensitising events in the second and third trimester, that would be indications for Anti-D in a Rh negative woman

Answer 7

Abdominal trauma
TOP
APH / Obstetric haemorrhage
Amniocentesis
ECV attempt

Question 8

When is routine Anti-D prophylaxis not required in the Rh negative woman in pregnancy?

Answer 8

Women is already sensitised i.e. has Anti-D antibodies
Fetal genotyping confirms the fetus is Rh negative
Father is confirmed to be Rh negative

Question 9

What is the pathophysiology of Haemolytic Disease of the Newborn?

Answer 9

Fetal RBCs enter maternal circulation and her immune system creates antibodies against these.

Trans-placental passage of maternal IgG antibodies into fetal circulation.

Antibodies cause fetal RBCs to be destroyed by their own immune system leading to HDFN.

Question 10

What is different about Anti-K HDN compared to Anti-D and Anti-c?

Answer 10

Anti-K: erythroid suppression, immune destruction of early erythroid progenitor cells

Severe fetal anaemia can occur at low antibody titres
Therefore, refer at any titre level

Question 11

What are the main three antibodies that can cause fetal anaemia, via HDN?

Answer 11

Anti-D
Anti-c
Anti-K

Question 12

What are five less common antibodies that can cause fetal anaemia via HDN?

Answer 12

Anti-E
Anti-Fy
Anti-Jk
Anti-C
Anti-c+E

Question 13

Which antibody potentiates the severity of fetal anaemia due to anti-c antibodies?

Answer 13

Anti-E

Therefore, if Anti-E present with anti-c, referral at lower titres is indicated

Question 14

What are the titres for Anti-D for mild risk, moderate risk and severe risk

Answer 14

Mild <4

Refer to fetal medicine if >4
Moderate: 4-15
Severe > 15

IU/mL

Question 15

What are the titres for Anti-c for mild risk, moderate risk and severe risk of fetal anaemia

Answer 15

Mild risk: < 7.5

Refer to fetal medicine if >7.5
Moderate risk: 7.5-20
Severe risk > 20

Question 16

In the presence of antibodies that can cause HDN, how often should the titres be measured?

Answer 16

Every 4 weeks until 28/40, then every 2 weeks

Once titres reach level required for referral, subsequent measurements is of doubtful significance

Question 17

In the presence of levels/titres of maternal antibodies associated with moderate / severe risk for HDN, what should the management be?

Answer 17

Weekly USS, specifically assessing for MCA PSV

MCA PSV

• predictive of moderate or severe fetal anaemia with 100% sensitivity and a false positive rate of 12%
• less sensitive after 36/40

Weekly USS can also assess for polyhydramnios, skin oedema, cardiomegaly

Question 18

If the MCA PSV > 1.5MoM in the context of maternal antibodies implicated in HDN, what is the management?

Answer 18

FBS
- measure Hb, bilirubin, DAT

Intra-uterine transfusion

Question 19

What did the Cochrane Review regarding Anti-D administration in pregnancy for preventing Rhesus alloimmunisation show?

Answer 19

Compared women given anti-D at 28/40 and 34/40 vs not

No clear difference in the risks of iso-immunisation
RANCOG Statement reads this as SHOWING a difference (but none were significant)

Question 20

What is the Cochrane Review evidence regarding postnatal Anti-D

Answer 20

Anti-D, given within 72 hours after childbirth, reduces the risk of RhD alloimmunisation in Rh negative women who have given birth to a Rh positive infant
Within six months of the birth and in their next pregnancy

Question 21

What is the Cochrane Review evidence regarding Anti-D administration after spontaneous miscarriage for preventing Rh alloimmunisation?

Answer 21

Insufficient data, small size

Until high quality evidence available, should follow local / national guidelines

Question 22

What is the Cochrane evidence regarding IV vs IM Anti-D?

Answer 22

Findings suggest they are equally effective

Low numbers, insufficient data

Question 23

What is mirror syndrome?

Answer 23

Rare complication of fetal hydrops
Association of fetal and placental hydrops
With maternal oedema and PET
“Triple oedema”

Oedema
Mild maternal hypoalbuminaemia
PET is unusual

Question 24

What is a rare maternal complication of fetal hydrops?

Answer 24

Mirror Syndrome

Question 25

What is the overall perinatal survival with red cell antibodies?

Answer 25

84%

Non-hydropic 94%
Hydropic 74%

Question 26

Outline the causes of fetal anaemia:

Answer 26

Infection:

• Parovirus
• CMV
• Toxo
• Syphilis

Immune:
- RBC alloimmunisation: Rh and other antigens

Inherited: metabolic diseases e.g. pyruvate kinase deficiency, G6PD deficiency.
- thalassaemia

Obstetric:

• MC twins: TAPS
• Feto maternal haemorrhage
• Down syndrome: transient abnormal myelopoeisis
• Maternal acquired red cell aplasia
• Vascular tumour e.g. chorioangioma
• AVM

Question 27

List the clinical implications of maternal red cell antibodies for mother and fetus

Answer 27

Fetus:

• Fetal, neonatal anaemia and thrombocytopaenia
• Fetal hydrops and perinatal death
• Preterm birth
• Late anaemia secondary to transfusion-mediated suppression of neonatal erythropoeisis.
• Hyperbilirubinaemia, jaundice, kernicterus and SNHL (toxicity 8th CN).
• Cholestasis: iron overload of liver from multiple transfusions.

Mother:

• Issues with timely provision of blood or blood components.
• Risk of alloimmunisation during FBS/IUT.

Question 28

Antenatal administration of Anti-D particularly for routine prophylaxis reduces the risk of alloimmunisation by what %?

Answer 28

80%

Question 29

What history would you want to know for a woman with clinically significant antibodies?

Answer 29

Cause of alloimmunisation:

• Blood transfusions
• Inadequate or omitted anti-D prophylaxis

Previous pregnancy outcomes:

• IUTs and gestation at which they were started.
• Gestation at delivery
• Neonatal anaemia
• Need for exchange transfusions or phototherapy

Relevant past history

Question 30

What causes fetal/neonatal alloimmune thrombocytopaenia?

Answer 30

Maternal-paternal platelet type incompatibility leading to maternal immune system making platelet specific antibodies.

Question 31

What is the incidence of FNAIT?

Answer 31

Rare 1 in 8000

Question 32

What history would you want to know from a woman with platelet specific alloantibodies?

Answer 32

Previous pregnancies affected (fetus or neonate) including:

• Intracranial haemorrhage and timing.
• Cord/newborn Plt count
• Maternal antiplatelet antibody investigations
• Any maternal therapies.

Question 33

What is the prognosis for FNAIT?

Answer 33

• 80% risk of recurrence if previous child affected and not treatment received.
• Tends to worsen with each pregnancy without treatment.

Question 34

What investigations are part of work-up for FNAIT?

Answer 34

• Maternal platelet specific alloantibodies
• Ultrasound to identify fetal ICH
• Maternal and parternal platelet typing and compatibility of both parents

Question 35

What test results would make you concerned this pregnancy is at risk of FNAIT?

Answer 35

Paternal platelet testing: heterozygous for particular antibody producing antigen. Tissue typing lab should be consulted for advice on invasive testing of pregnancy to tissue type the fetus.

If fetus is compatible with the mother, ongoing treatment and surveillance is not required.

Question 36

What is the antenatal management of FNAIT

Answer 36

• Sibling without ICH: start weekly IVIG from 28 weeks, dose 0.5g/kg.
• Sibling WITH ICH: start weekly IVIG from 16 weeks, dose 1g/kg.
• Fetal ICH diagnosed but pregnancy continuing: weekly IVIG, dose 1g/kg.
• Consider steroids for high risk women however lack of evidence it improves Plt counts.

Fetal ICH diagnosed: for fetal brain MRI and MDM. Options to continue pregnancy or terminate.

Question 37

What is the role of FBS and IUPT?

What is the issue with IUPT?

What are the risks?

Answer 37

Reserved for time of delivery planning.
Transfusion threshold Plt count <30 x <30 x 10^9/L.
Should be considered pre-CS if sibling had ICH.
Needs to be performed in setting where immediate CS can be performed.

Issue: tranfused platelets have short half-life 2-5 days unlikely RBCs.

Risk of fetal bleeding from puncture site.

Question 38

What is the recommended timing and mode of delivery for FNAIT fetuses?

Answer 38

• Sibling without ICH: elective IOL at 37 weeks. Should avoid FSE, FBS and instrumental deliveries.
• Sibling with ICH: elective CS at 36 weeks. Consider pre-CS FBS and IUPT.
  IOL considered if strong maternal wish.
• This fetus diagnosed with ICH: elective CS at 34 weeks.