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FETAL DIAGNOSES & TREATMENT
During the
birthing process, blood cells from the
unborn child can escape into the mother's
bloodstream. These cells are recognized as
foreign if they are a different blood type
from the mother and a natural rejection
process will ensue with the formation of
antibodies. The process is known as red cell
alloimmunization.
This event
typically occurs after the delivery of a
baby at the end of pregnancy, but other
pregnancy-related events such as elective
abortion or spontaneous miscarriage can
result in antibody formation. Although the
pregnancy in which the alloimmunization
first occurs results in an unaffected child,
future children are at substantial risk. In
these subsequent pregnancies, newly formed
antibodies in the pregnant patient can cross
to the unborn child and attach to its red
blood cells producing a low blood count
(anemia) and in the worst case scenario,
fetal death. These antibodies can be
measured in a woman's bloodstream by a test
called an indirect Coombs or antibody titer.
In general, the fetus of each subsequent
pregnancy exhibits more severe effects than
in the previous pregnancy. The fetal and
newborn effects of red cell alloimmunization
are known as hemolytic disease of the
newborn.
In more than 98 percent of cases, the red
blood cell incompatibility involves the
Rhesus or Rh D antigen so the disease is
known as Rhesus disease or Rh disease.
Although the exact percentage varies with
race, 15 percent of the United States
population is Rh-negative and 85 percent is
Rh-positive. If a Rh-negative woman
conceives a child with a Rh-positive
partner, the potential exists for the child
to inherit its father's Rh-positive blood
type. There are two types of Rh-positive
men. In 55 percent of people, the man is
heterozygous. In this situation, his
genetics allow him to produce Rh-negative
offspring 50 percent of the time and
Rh-positive offspring the remaining 50
percent of the time. In the second type of a
Rh-positive individual, only Rh-positive
offspring can result, a condition known as
the homozygous state.
Data from the Centers for Disease Control
(CDC) indicate that the incidence of
hemolytic disease of the newborn secondary
to Rhesus disease is approximately one case
per 1000 live born infants.
Medication is available to prevent Rhesus
disease. Rhesus immune globulin (also known
as RhoGAM) should be administered to the
Rh-negative woman with a Rh-positive partner
any time there is a chance fetal cells may
enter the pregnant woman's circulation. Such
events include threatened miscarriage,
spontaneous miscarriage, ectopic pregnancy,
chorionic villus sampling or amniocentesis
performed for genetic indications, and motor
vehicle accidents. Rhesus immune globulin
should be administered routinely at 28 weeks
of pregnancy and after the delivery of an
Rh-positive infant. If given correctly, this
medication is more than 99 percent effective
in the prevention of Rhesus disease. Rhesus
immune globulin is only effective in
preventing Rhesus disease; it is not
effective in preventing worsening disease
once alloimmunization has occurred.
Unfortunately, similar medications are not
available to prevent alloimmunization to
other more rare red cell antigens such as
Kell.
In 75 percent of first affected pregnancies,
the pregnancy can be followed with serial
antibody measurements taken from the
pregnant patient's blood. These
are called antibody titers. As long as the
titer remains below a critical value
(usually 1:32), no additional testing is
required. In the remaining 25 percent of
first affected pregnancies, a high maternal
titer will mandate such invasive fetal
testing as amniocentesis to measure the
amount of bilirubin, an indirect assessment
of the rate of breakdown of fetal red blood
cells, in the amniotic fluid. Amniocentesis
is performed by directing a needle with
ultrasound into the fluid-filled space that
surrounds the fetus. In a few select cases,
it may be necessary to obtain blood directly
from the fetal umbilical cord to assess the
degree of anemia in the baby while it still
remains in the womb. This procedure is known
as cordocentesis or percutaneous umbilical
blood sampling.
In 12 percent of first affected pregnancies,
the infant may require intrauterine
transfusions. In this procedure, a needle is
directed under ultrasound guidance into the
umbilical cord and blood is infused directly
into the fetus to correct its anemia. The
procedure is usually repeated at 2 to 3 week
intervals for the remainder of the pregnancy
until approximately 35 weeks of the
pregnancy. The survival rate after
intrauterine transfusion is approximately 85
percent.
Red cell alloimmunization secondary to non-RhD
antibodies continues to be a problem since
prophylactic immune globulin is not
available to prevent these cases. Although
the RhD antigen causes more than 98% of all
cases of hemolytic disease of the newborn,
more than 43 other red cell antigens have
been implicated. Especially problematic are
the Kell (K1), c, Duffy (Fya), and Kidd (Jka
and Jk b) antigens. A recent study from a
tertiary referral center in New York found
550 cases of antibodies associated with
hemolytic disease of the newborn in 37,506
blood samples taken from women of
reproductive age (1.1 percent incidence).
Anti-D occurred in 25 percent of the
samples, anti-Kell in 28 percent, anti-c in
7 percent, anti-Duffy in 7 percent,
anti-Kidd in 2 percent, anti-E in 18
percent, anti-C in 6 percent, anti-MNS in 6
percent, and anti-Lutheran in 2%.
The majority of cases of Kell sensitization
in the United States are secondary to
incompatible red cell transfusions since
blood is not routinely cross matched for the
Kell antigen. In the case of the Kell
antigen, 92 percent of males will be Kell
negative; only Kell negative, unaffected
offspring can therefore be expected if these
individuals father a child. For this reason,
Kell typing of the father is the primary
step in the management of Kell disease in
pregnancy. The remaining 8 percent of males
will be Kell positive; 98 percent of these
will be heterozygous while 2 percent will be
homozygous. In the case of the little c
antigen, 80 percent of males will be
positive for the antigen and 50% will be
heterozygous.
Kell disease in pregnancy is managed more
aggressively than Rh disease due to several
reported cases of severe fetal anemia with
low maternal antibody titers. A titer of 1:8
instead of 1:32 is used to decide when to
begin invasive testing. Amniocentesis for
bilirubin determination is NOT reliable in
cases of Kell disease therefore most authors
would use cordocentesis to directly test for
fetal anemia. Due to the infrequency of the
other non-RhD red cell antibodies, most
centers use diagnostic and treatment
protocols similar to Rh disease. A critical
titer of 1:32 is used to indicate when such
invasive testing as amniocentesis or
cordocentesis is warranted.
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