-
Causative organism: Cytomegalovirus, a ubiquitous DNA
herpes virus.
-
Most common cause of perinatal infection.
-
Incidence: fetal infection found in 0.2 to 2% of all
newborn infants.
Transmission:
-Horizontal transmission by
droplet infection via saliva and urine.
- Vertical transmission by mother
to fetus – infant.
- Sexual transmission.
- After primary infection the
virus becomes latent. Periodic reactivation with viral shedding is possible
despite of the presence of serum antibody.
Immunosuppressed states increase
the propensity of serious cytomegalovirus infections.
Features of maternal infection:
-
No evidence that pregnancy increases the risk or
severity of maternal CMV infection.
-
Most of the infections will remain asymptomatic. About
15% of the adults will have mononucleosis like syndrome.
With features like :
-
Fever
-
Pharyngitis
-
Lymphadenopathy
-
Polyarthritis.
-
The risk of sero-conversion among susceptible women
during pregnancy is 1 to 4%.
-
In around 40% cases primary infection to the fetus is
associated with severe morbidity.
-
Transmission is more common in first half of the
pregnancy.
-
Maternal immunity to CMV does not prevent recurrence or
reactivation or congenital infection.
-
Usually recurrent infections are more common cause of
congenitally infected newborn.
-
Fortunately clinically apparent sequelae are less
common with recurrent infections than primary infections.
Congenital infection:
-
Results in cytomegalic inclusion disease.
-
This syndrome presents with features like low birth
weight, microcephaly, intracranial calcifications, chorioretinitis, mental and
motor retardation, sensorineural deafness, hepatosplenomegaly, jaundice,
hemolytic anemia and thrombocytopenic purpura.
-
Usually these findings are seen in 5 to 6% of infected
neonates only.
Daignosis:
Infection is diagnosed by measuring IgG and IgM antibodies.
If patient results show :
-
IgG and IgM negative
- indicates Cytomegalovirus uninfected and no further evaluation is
needed.
-
If abnormal Cytomegalovirus screening with IgG and IgM
positives occur, following steps are needed, estimation of:
-
CMV specific IgG and IgM by EIA.
-
CMV specific IgG avidity by EIA.
-
CMV specific IgM by immunoblot.
Then if the results show:
-
CMV IgG positive, high IgG avidity index and IgM
negative- latent CMV infection. And no further evaluation is needed.
-
CMV IgG positive or serocenversion, low IgG avidity
index and IgM positive – primary CMV infection. Needs invasive follow-up.
-
Uncertain serologic results – undefined CMV infection.
Needs invasive follow-up.
-
CMV IgG positive, high IgG avidity index and IgM
positive – recurrent CMV infection. Needs non-invasive follow-up.
-Ultrasound to know the effects on the fetus. Sometimes
defects like microcephaly, ventriculomegaly, cerebral calcifications,
hyperechoic bowel, ascites, hepatosplenomegaly and hydrops etc. can be seen.
-Amniotic fluid analysis using viral culture and polymerase
chain reaction.
-Fetal blood sampling- to detect anemia, thrombocytopenia,
hepatic dysfunction etc.
-The fetal outcome depends on the stage of gestation during
which primary infection documented.
-Usually the majority of infants develop normally even with
being affected with primary infections in the first half of the pregnancy.
Treatment:
-No effective therapy for maternal infections. So routine
serological screening is not recommended.
-Not possible to predict which fetuses are infected.
-Maternal reinfection with a different CMV strain can occur.
-No vaccine.
-Attempts to identify and isolate infants excreting CMV are expensive and impractical.
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