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Alloimmunization disorders

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Title: Alloimmunization disorders

1
Alloimmunization disorders

Steven R. Allen, MD
Scott White Hosp Clinic
Temple, TX

2
Educational objectives

Review fetal neonatal consequences of
alloimmunization disorders
Update genetics of Rh blood group
Discuss strategies for prevention of Rh
alloimmunization
Develop management strategies for
alloimmunization disorders

3
Immune responsesAb against Ag from

Autoimmunity
Isoimmunity
Alloimmunity
Heteroimmunity

Self
MZ twin inbred strain
another member, same species
another species

4
Alloimmunization Disorders

Rhesus blood group
Atypical blood groups
Platelet

5
Rh alloimmunizationHistoric landmarks
1940 Rhesus similar human RBC Ag
(Landsteiner Weiner)
1992 RhD non-D cloned
1932 hemolysis assocd with hydrops (Diamond)
1963 IP trans (Liley)

1938 a-fetal Hgb Ab postulated (Darrow)
1961 AF bili predicts HDN severity (Liley)
1985 PUBS trans (Daffos)
1600s hydrops, jaundice unknown etiology
1967 RhIG
6
Rh alloimmunizationHistoric landmarks
1940 Rhesus similar human RBC Ag
(Landsteiner Weiner)
A Success Story
1992 RhD non-D cloned
1932 hemolysis assocd with hydrops (Diamond)
1963 IP trans (Liley)

1938 a-fetal Hgb Ab postulated (Darrow)
1961 AF bili predicts HDN severity (Liley)
1985 PUBS trans (Daffos)
1600s hydrops, jaundice unknown etiology
1967 RhIG
7
Rh genetics biochemistry

Rh D and more
2 homologous structural genes on 1p36-p34, RHD
(encoding D) RHCE (encoding CcEe polypeptides),
with 92 sequence identity
Alternative mRNA splicing of single gene produces
CcEe Ag variability

8
Rh genetics biochemistry

Gene product 417 AA non-glycosylated hydrophobic
transmembrane protein, expressed only on
erythrocytes (unknown function, and no shared
sequence homology with any other known protein)
Other blood groups encoded on chromosome 1 and
other chromsomes

9
Rhesus blood group
10
What is Du?

Present in 0.2-1 of caucasians
Prior Du designation has been changed to weak D
positive
Created by a variety of mutations in RhD gene
Manage as if D positive

11
Incidence of Rh negativity

a caucasian trait
12
Development of Rh alloimmunization

Rh neg mother
Maternal exposure to Rh pos RBCs
non-pregnant transfusion, including RBC
contaminated plts or WBCs
pregnant transplacental hemorrhage (dose
dependent incidence follows)
75 overall
60 ? 0.1 mL (0.1 mL sufficient for
alloimmunization)
0.25 gt 30 mL

13
Maternal immune response D alloimmunization

Primary
weak
IgM (IgG wks later)
develops over 8 wks to 6 mos

Secondary
rapid response of IgG
higher avidity than primary response

Maternal response modulated by ABO status ABO
incompatibility is protective (alloimmunization
risk decreased by 75)
14
Risk of Rh alloimmunizationP0, Rh neg mom, Rh
pos fetus, ABO compatibleno RhIG

90 due to peripartum feto-maternal hemorrhage
15
Risk of Rh alloimmunizationP0, term preg, Rh
incompatible, ABO compatibleEffect of RhIG

0.1
16
Mechanism of hemolytic disease of the newborn
(HDN)

Fetal RBCs destroyed by mat ?-D (IgG)
non-complement mediated
?-D coated RBCs adhere to macrophages, form
rosettes, are trapped in spleen
RBC membrane fragments removed, with RBC
fragility lysis
Fetal anemia

17
Mechanism of hemolytic disease of the newborn
(HDN)cont

Extramedullary erythropoiesis
erythroblastosis
hepatosplenomegaly
hep dysfxn, including hypoproteinemia
portal hypertension
Hydrops

18
Rh Immune Globulin

300 ?g dose neutralizes exposure risk of up to 30
mL fetal blood if given within 72 h
AABB recommends screen before each dose (to r/o
greater exposure volume or prior
alloimmunizaiton)
t 1/2 24 dgenerally effective for 12 wk
(if given _at_ 28 wks, 15-20 will have low titer _at_
term)
risk of viral infxn minimal (Hep C) to absent
(HIV)

19
Prevention of Rh AlloimmunizationACOG RhIG
recommendations (Level A)

Rh neg women not Rh alloimmunized should receive
RhIG
At approx 28 wks (unless FOB Rh neg)
Within 72 h of del of Rh pos infant
After a 1st TM pregnancy loss
After invasive procedures, such as amniocentesis

Prac Bull 4, 5/99
cost-effective
20
Prevention of Rh AlloimmunizationACOG RhIG
recommendations (Level C)

RhIG prophylaxis should be considered if a
patient experiences
threatened abortion
2nd or 3rd TM bleeding
External cephalic version
Abdominal trauma

Prac Bull 4, 5/99
21
Advantage to Rh immunoglobulin admin after BTL?

Some women later want a pregnancy
Improves availability of blood if a transfusion
ever needed

22
Screening for Rh Alloimmunization

1st TM Rh IDC
If Rh pos, no further testing indicated
If Rh neg IDC neg, give RhIG at 28 wks (and rpt
IDC per AABB recommendation)
If Rh neg IDC pos, check titer serially, q
2-4 wks (mgmt based in part on titer)

23
Predictors of severity of HDN

Rhesus genotype of father of baby
History of HDN
Maternal Ab titer
Amniotic fluid spectrophotometric measurements
Ultrasonographic findings
MCA peak velocity
hydrops
Invasive fetal testing

24
Rhesus genotype of father of baby

Rh neg NO RISK - routine prenatal care
(regardless of maternal ?-D titer)
Rh positive
Zygosity for D can be predicted based on CcEe
phenotype or genotype, ethnicity, and number of
prior D-positive offspring
if homozygous (45), then fetus at risk
if heterozygous (55), fetus has 50 chance of
being vulnerable
Assume Rh pos ( fetus at risk) if unable to
confirm otherwise

25
History of HDN

Subsequent pregnancies generally have similar or
gt degree of alloimmunization
Risk of recurrent hydrops 90
Hydrops generally recurs at similar or earlier
(not later) gestational age
Risk of hydrops in 1st affected pregnancy 10

26
Maternal ?-D titer

?-D titer is a crude predictor
Critical titer indicates the need for additional
evaluation
Critical titer generally 16
(altho may vary, 8-32, between labs and by
technique)

27
Ultrasonography to assess for fetal anemia

Hydrops is a late sign of significant anemia
Doppler velocimetry predicts anemia - best
studied in MCA
peak velocity gt 1.5 MoM for gest age predicts
anemia (sensitivity ? 86 false pos rate 12)

NEJM 20003429-14
28
Invasive fetal testing

Amniocentesis
?OD 450
fetal Rhesus genotype
Umbilical blood sampling
reserved for those at risk for severe anemia
(based on non-invasive testing)

29
?OD 450 (correlates with bilirubin concentration)
Wavelength (nm)

OD
?OD 0.21
30
Liley graph
Gest age (wks)
Potential for fetal death in 7-10 d
3
?OD 450
2
1
Low risk of significant anemia
31
Limitations to ?OD 450interpretation

Original Liley graph limited to gestational ages
? 28 wks
Physiologic (nl) fetal bilirubin production peaks
at 23-25 wks
Poor correlation between ?OD 450 and fetal Hct lt
28 wks
Betamethasone may artifactually lower ?OD 450

32
Fetal blood analysis

Direct degree of anemia
lowest normal Hct 30 (18 wks) to 33 (30 wks)
hydrops rarely occurs above 15 Hct
Indirect correlates of anemia
reticulocyte count
Direct Coombs titer

33
In utero transfusion

Rationale for therapy
suppression of abnormal erythropoiesis
improvement of O2 carrying capacity
prevention of hydrops
opportunity for pulmonary maturation
Blood for transfusion
O negative, compatible with mother
washed, irradiated, CMV negative
tightly packed (Hct approx 85)

34
Intraperitoneal transfusion

EGA gt18 wks
RBCs absorbed into fetal circulation, 12 per day
larger transfusion volumes allow longer intervals
between transfusions
generally replaced by IVT

35
Intravascular transfusion

EGA gt 18 wks
transfuse max of 30-50 mL/kg
repeat at intervals based on fetal status, final
Hct, and expected decline of Hct (1 per day)
better results than IPT if anterior placenta or
fetus hydropic

36
Prognosis for survival following transfusion

Intraperitoneal
9 (if transfusion required before 25 wks) to
49 (includes hydropic fetuses) to
84 (best reported)

Intravascular
82 (hydropic) to
89 (non-hydropic) to
96 (best reported)

?
37
Suppression of Alloimmunization

Not effective
Promethazine
Oral Rh RBC membranes
RhIG

Limited/potential benefit
Plamsapheresis
IVIG
begin 1st TM may delay need for invasive
testing

38
Predictors of severity of HDN

Rhesus genotype of father of baby
History of HDN
Maternal Ab titer
Amniotic fluid spectrophotometric measurements
Ultrasonographic findings
MCA peak velocity
hydrops
Invasive fetal testing

39
Start here if prior hydrops paternal Rh
positive
40
Case 1

28 yo P1001 (uncomplicated prior preg)
Anti-D titer rising to 16 _at_ 16 wks
Husband Rh pos (prior baby Rh pos recd rhogam
_at_ 28 wks p/partum no hx of transfusion or
other exposures)
Amnio _at_ 24 wks fetus D pos (and delta OD450
extrapolated to mid Zone 2 of Liley curve)

41
Liley graph
Gest age (wks)
3
?OD 450
2
1
42
Case 2

21 P2022
Anti-D titer 256 _at_ LOC, 30 wks
Unmarried new partner unaware of Rhogam given
for last preg/EAb
FOB not available for testing

43
Liley graph
Gest age (wks)
3
?OD 450
2
1
44
Case 3

31 yo P3103
Last pregnancy was delivered _at_ 34 wks for hydrops
(neonatal demise from HDN)
Current husband father of all her children one
prior Rh neg child
Anti-D titer?

45
Liley graph
Gest age (wks)
3
?OD 450
2
1
46
Atypical Blood Group Alloimmunization

Accounts for 2-5 of HDN increasing as Rh
alloimmunization becomes less common
Develops after blood transfusion
RBCs for transfusion compatible only for ABO D
incidence of sensitization 2 after transfusion
Incidence 2 in general Ob population

47
Examples of atypical alloimmunization

Fetal risk
Kell (K)
Duffy (Fya)
Kidd (Jka)
M
S

Benign
Lewis (Le)
I
P
Duffy (Fyb)

Extensive list - use reference chart
48
Management of Atypical Alloimmunization
(-)
()
(-)
( or unknown)
Kell suppresses erythropoeisis - greater
anemia PUBS sooner
49
Neonatal alloimmune thrombocytopemia