Fetal anemia
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Transcript Fetal anemia
ISOIMMUNISATION
William 2001
I.
II.
III.
IV.
V.
VI.
VII.
Fetal anemia
Fetomaternal hemorrhage
Isoimmunisation
Immune hydrops
Management
Pervention
Large fetomaternal Hge
FETAL ANEMIA
Normal fetal Hb% > 35 weeks = 17 gm/dL
Fetal anemia = < 14 gm/dL
Causes:
Placenta cut or torn
Fetal vessel perforation
Raising the neonate above the abdomen
of his mother before clamping the cord
Delayed clamping of the cord ↑ of
fetal Hb by 20%
FETAL-TO-MATERNAL HEMORRHAGE
Common in all pregnancies
Rarely > 30mL = 0.3 – 0.6%
Benefit in fetal karyotyping
Keihauer – Batke test:
Identify fetal RBCs by acid elusion
darker than maternal RBCs
Rosette test:
Maternal blood + anti D Ab+ indicator
fetal blood surrounded by Abs
More accurate in hemoglobinopathy
Severe anemia sinusoidal FHR
not pathognomonic
evaluate immediately
Chronic anemia may normal FHR
Significant acute /chronic Hge may
Neurological impairment due to:
Hypotension ↓ perfusion
Ischemia
CNS infarction
Obstetric management may not
improve CNS damage
Large fetal Hg may fetal death
in 5% and the cause may be unknown
e.g. chorioangioma
Placental abruption :
usually mild Hg
except if traumatic
Quantification of volume of blood loss:
influence management
Determine the dose of Anti D Ig
Fetal red cells =
maternal Hct
X maternal blood volume
X % of fetal cells in Kleihauer
- Batke test ÷ neonatal Hct
Causes of fetal-to-maternal Hg:
Early abortion
Elective abortion
Ectopic
Amniocentesis
Cordocentesis
Chorionic villous sampling
Antepartum trauma
Placental abruption
Fetal demise
Manual placental extraction
External version
ISOIMMUNISATION
ABO blood group
CDE blood group
Other blood groups
Kell antigen
Other antigens
History:
1892 Ballantin hydrops fetalis
1932 Anemia and reticulosis are
present in hydrops fetalis
1940 Landsteiner & Weiner
Rh factor
1941 Levein hydrops is caused
by maternal isoimmunisation
by Rh –ve fetus
1961 Anti Rh
- Fetal blood contain > 400 Ags
most of them are insignificant
- Most people inherit at least 1 Ag
from their fathers that is lacking
in their mothers
- Isoimmunisation of an Rh –ve
pregnant woman occur as a
result of:
Rh +ve fetus
Blood transfusion
Isoimmunization is rare because:
Variable Ag amounts
Variable antigenicity
Maternal immune respond
↓ placental passage
ABO incompitability
destruction of fetal RBCs
Not all isoimmunization hydrops
2% of all women are isoimmunized
6 months postpartum
% of isoimmunisation with Rh-ve
ABO compatible fetus:
2% at delivery
7% 6 months postpartum
7% next pregnancy
Total = 16%
ABO blood group incompatibility:
- The most common cause of hemolytic
disease of the neonate
- 20% of all fetuses are ABO incompatible
only 5% of them are clinically affected
- Mild anemia & ↑ reticulocytes
- No erythtoplastosis
- Treated by phototherapy
Difference from Rh incompatibility:
Affect 1st baby
Milder ( Ig M does not pass placenta)
Rarely progressive
Affect African Americans
Criteria of ABO incompatibility:
1st day jaundice
Mother O, fetus A,B,or AB group
Anemia, ↑ reticulocytes
Management of ABO incompatibility:
Same as Rh isoimmunization but:
No amniocentasis
No blood transfusion
Because there is no hydrops
CDE blood group:
5 types: c, C, e, E, D
- D is +ve if present and –ve if absent
- D isoimmunisation is the most common
isoimmunization
- D –ve pregnant women are sensitized if
their fetus is D +ve
- CDE genes are inherited independent on
other blood groups
- They are located on chromosome 1
Geographic distribution of D +ve
populations:
Native Americans
and Chinese
95%
African Americans
92%
Caucasians
87%
Basque
76%
Other blood groups: % = 1
- ¼ Lewis blood group mild
jaundice starts weeks postpartum
- 74% D, C, c, E & e antigens
- Recently Rh isoimmunization is ↓
due to Anit D treatment
- Now Rh
= 40%
Other Ags = 60%
Kell antigen:
- Caucasian kell +ve = 91%
- Isoimmunisation occur by pregnancy
or blood transfusion
- Much earlier and more severe
anemia which can not be predicted
by:
Maternal titer
AF bilirubin = mild/moderate
- May fetal death inspite of:
Blood transfusion
Normal AF bilirubin
- Hemolysis ↓ due to:
↓ RBCs
↓ bilirubin
- If maternal anti-Kell Ab titer ≥ 1 : 8
Cordiocentesis because AF bilirubin
is out of proportion to anemia
Other antigens:
Kid Ag:
Jk a –ve = 25%
Jk b –ve = 25%
Jk a - b +ve = 50%
Duffy Ag:
Fy a – b –ve in some blacks
C Ag:
Most common Ag after D
Moderate to severe hemolysis
IMMUNE HYDROPS
Immune hydrops
Hyperbilirubinemia
Mortality
Identification of
isoimmunization
Fetal Rh genotype
IMMUNE HYDROPS
RBCs hemolysis by isoimmunization
Hyperplasia of BM
Hyperplasia of extramedulary
sites:
Liver
Spleen
Liver:
Fatty degeneration
Deposition of hemosidrine
Large canaliculi with bile
Heart: HF
Lungs: Hge - immature
When fluid accumulate in subcutanous
tissues hydrops fetalis
Definition:
Abnormal fluid in ≥ 2 sites:
Ascitis – oedema – pleural effusion
Placenta:
Enlarged cotyledons
Odemotus villi
Boggy
Fetus:
Dystocia due to:
Hepatospleenomegaly
Odema
PATHOPHYSIOLOGY
Heart:
HF hypoxia capillary leakage
Extramedulary hyperpleasia:
Hepatic parynchemal distruction
portal HTN
umbilical vein HTN
Liver disease:
↓ protein
↓ colloidal osmotic P
Study:
Cordiocentesis in hydrops:
Hb = < 3.5 gm/dL
Plasma protein = < 2 SD
AF plasma protein ↑
The degree of anemia affect
the degree of ascitis and made
worse by ↓ plasma proteins
Capillary endothelial damage:
Capillary leakage
↓ protein
Study:
↑ Umbilical vein pressure is due to
cardiac dysfunction and not
portal HTN
Sinusoidal FHR = impending death
Neonate:
Pale
Edematous
Limp
↑ need for resuscitation
Dyspnea
Collapse
Hepatospleenomegaly
Petechiae
ecchymosis
HYPERBILIRUBINEMIA
Less affected fetuses are born
normal jaundice within hours
If untreated kernicterus = CNS
damage affecting basal ganglia
Mortality:
Reduced dramatically due to:
D Ig
Blood transfusion
Induction of labor
IDENTIFICATION OF ISOIMMUNIZATION
Maternal serum Abs:
Unbound to RBCs disappear
within 1 – 4 months
Indirect Coombs T
Fetal serum Abs:
Bound to RBCs hemolysis
Direct Coombs test
Neonatal blood group:
Inaccurate because D-Ag may
be coated with D-Ab
If maternal Abs are present:
Ig G or Ig M ?
(Ig M can not pass the placenta)
If Ig G antibody titer:
< critical value 1 : 16 repeat
> critical value 1 : 16 evaluate
Critical values for other Ags:
Kell ≥ 1 : 8
C, E ≥ 1 : 32
The presence of Abs in the
mother does not mean that:
The fetus is +ve
He will be affected
Amnestic response:
= ↑ Ab titer + Rh –ve fetus
Because ½ of adult males are
heterozygous for D Ag
¼ of women at risk are Rh -ve
Estimation of fetal genotype:
The father is tested for:
Blood group
Most likely arrangement of his CDE
genes = presumed genotype based
on the most common arrangement
of genes in men of his race
If the father is white:
94% chance to be heterozygous
47% chance of having D –ve fetus
MANAGEMENT
Amniotic fluid evaluation
Expanded Liley graph
Fetal blood sampling
Subsequent child development
Other methods to ↓ hemolysis
Delivery
Exchange transfusion
Prevention
Routine antepartum anti-D
AMNIOTIC FLUID EVALUATION
↑ Hemolysis ↑ AF bilirubin
↑ anemia
Since AF bilirubin is very small
measured by a continuously recording
spectrophotometer and is demonstrable
as a change in absorbance at 450 nm
( ∆ OD 450 ) then the results are
plotted on Liley graph (1961)
LILEY GRAPH
Zones of Liley graph:
Zone 1 = mild anemia
= 14 gm %
Zone 2 = moderate/severe anemia
= 13.9 – 8 gm %
Zone 3 = severe anemia
= < 8 gm %
= death in 7 – 10 days
If the results are in zone 1 or 2:
repeat in 1 – 2 weeks and draw
a line between the 2 results:
- If the trend of the line is:
Decreasing
Parallel to the lines of the graph
= unaffected fetus or stable
repeat / 2 – 3 weeks until
transfusion or delivery
- If the trend of the line is:
- Rising within the zone
- Rising to zone 3
= Unstable
Managed as zone 3
If the results are in zone 3:
= Severe anemia
Immediate blood
transfusion or delivery
Expanded Liley graph:
Since Liley graph was made for fetuses
> 27 week, expanded graph back to
18 – 20 weeks is inaccurate, because
AF bilirubin < 25 weeks is high
So, in cases of:
Hydrops
< 25 weeks
Severe anemia < 25 weeks
It’s better to do cordocentesis
FETAL BLOOD SAMPLING
Cordocentesis is risky # amniocentesis
Advantages: blood typing
Recently amniocytes for Rh typing:
100% accurate
99.7% sensitivity
94% specificity
Also for C,E , Kell & other Ags
If fetus is Rh–ve no further tests
If amniocentesis possible anemia
U/S
hepatomegaly
NST/BPP
fetal stress
immediate blood
transfusion or delivery
Tests of cordocentesis:
Hb%
HTV
Indirect Coombs titer
Reticulocyte count
Indications of IU blood transfusion:
Hb 2 gm/dL < mean of normal
Hb in the fetuses in the same GA
HTV 30% = 2 SD < mean at all GAs
Methods of intrauterine blood transfusion:
Intraperitoneal - intraumbilical
Subsequent child development:
90% normal – delayed - abnormal
Other methods to ↓ hemolysis:
Plasmapheresis
Large dose of promethazine
Corticosteroids for immunosuppresion
D +ve erythrocyte membrane capsules
All are ineffective
DELIVERY
Aim:
= Delivery at or near term
Monitor by fetal wellbeing tests
If the fetus is very immature:
Intrauterine blood transfusion
If near term: deliver
If lungs are mature induce labor
If compromised fetus CS
EXCHANGE TRANSFUSION IN THE
NEWBORN
If the mother is sensitized
cord blood sample for:
Hb%
Direct Coombs test
If overtly anemic exchange blood
transfusion by O –ve fresh blood
If not overtly anemic the need for
blood transfusion is determined by:
The rate of bilirubin ↑
Maturity
Complications
PREVENTION
By anti D Ig = 7S Ig G = 300 μg D Ab
Given within 72 hours of delivery
To none sensitized mothers only
Given after: abortion, mole, ectopic,
miscarrage
Rate of sensitization without D Ig:
2% of spontaneous abortion
5% of elective abortion
6% of amniocentesis
ROUTINE ANTEPARTUM
ADMINISTRATION
At 28 weeks
For all Rh –ve pregnant women
↓ isoimmunization from 1.8 % to 0.07%
In the past :
2nd injection 34 weeks
½ life of Ig :
= 24 hours Reduce titer by time
weak +ve indirect Coombs test
Now the 2nd injection is given if:
Fetomaternal Hg occurs
Amniocentesis > 3 weeks
from the 1st injection
The 2nd dose is against:
15 mL of D +ve RBCs
30 mL of fetal blood
Sometimes Ab cross the placenta
Weakly +ve direct Coombs test
Recognized by:
No anemia
No hyperbilirubinemia
Risk of transmission of diseases:
HIV inactivated by the factory
hepatitis patients are excluded
from donation very low risk
LARGE FETAL–TO - MATERNAL HG
Rarely 1 dose of Anti D Ig is insufficient
= Very rare occur 1 : 1250 deliveries
To avoid this all Rh –ve women should
be tested after delivery by Kleihaure Batke or rosette tests
Number of ampoules:
= fetal blood/15
Du antigen:
A variant of D antigen:
Du +ve & Du -ve
Less antigenic
Treated as Rh D –ve
Maternal to fetal Hg:
Very rarely an Rh –ve female fetus
is sensitized inutero by her mother
= Grandmother theory
No need for Anti D prophylaxis