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Cytomegalovirus infection

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CMV in Immunocompromised children Complications in AIDS patients: Retinitis. Esophagitis , Colitis , Hepatitis. Encephalitis,peripheral neuropathy. Pneumonitis. – PowerPoint PPT presentation

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Title: Cytomegalovirus infection


1
Cytomegalovirus infection
  • Presented by Dr.D. Al-Masri.
  • Moderated byDr.Y.Abu-Osbaa.

2
Introduction
  • It is the most common congenital infection in
    USA.
  • It is a leading cause of hearing loss,mental
    retardation, and cerebral palsy.
  • It is an opportunistic pathogen in
    Immunocompromised.

3
Introduction
  • It is a double stranded DNA virus.
  • It is the largest member of herpesviridae
    family..
  • Exit the cells by pinocytosis.
  • Restriction endonuclease.

4
Epidemiology
  • The prevalence of CMV infection and the age at
    first infection vary according to living
    conditions,child rearing practices, and sexual
    behavior.
  • Virus is present in saliva,tears,semen,urine,cervi
    cal secretions, and blood for months to years
    after initial infection as well as the milk of
    seropositive mothers.

5
Epidemiology
  • It has a worldwide distribution.
  • Prevalence
  • Health care providers are not at increased risk
    of infection from patients.

6
Epidemiology
  • It is transmitted via direct contact with body
    fluids, intimate contact, care of young children,
    blood transfusion, and organ transplant.
  • Congenital CMV infection occurs in approximately
    0.5 to 1.5 of births. It is well known that CMV
    can be transmitted to the fetus even when
    maternal infection occurred long before
    conception.

7
Epidemiology
  • It occurs in immune mothers due to reactivation
    of latent virus during pregnancy ,chronic
    infection, or reinfection with a new strain.
  • When primary infection occurs during pregnancy
    the risk of transmission to the fetus is 35. It
    occurs either by sexual contacts or contact with
    young children regardless of the gestational age.
  • Intrapartum transmission or transmission by human
    milk occur more commonly than congenital
    infection.
  • Infants who acquire the virus shed it in saliva
    and urine for years.

8
Pathogenesis
  • CMV is large complex virus that has 20 times the
    genetic material of HIV with DNA sequences
    encoding more than 100 proteins.
  • The infection occurs due to impairment of T-cell
    immunity.
  • Cytomegalic cells pathognomonic.

9
Pathogenesis
  • Important features in pathogenesis
  • Ability of the virus to destroy host cells.
  • Ability to infect wide range of cells and tissues
    .
  • Ability to to evade and interfere with host
    defense mechanisms.
  • Ability to persist indefinitely in the host.

10
Pathogenesis
  • Impaired organ function results from combination
    of lytic infection of cells and vascular
    compromise .
  • Dissemination is due to infection of WBC and
    vascular endothelial cells.
  • A small proportion of circulating monocytes in
    seropositive persons harbor latent CMV.

11
Pathogenesis
  • The ability of the virus to maintain active
    infection is due to
  • Inhibition of host cytotoxic T-lymphocyte
    responses by interference with processing and
    presentation of viral antigens by MHC class I
    molecules.
  • Interference with helper T-cell responses by
    degradation of MHC class II molecules.
  • Inhibition of killing by natural killer cell.
  • Interference with apoptosis and
    complement-mediated lysis or sequestration of
    chemokines.

12
Clinical manifestations
  • Mostly asymptomatic.
  • CMV accounts for 50 of cases of
    heterophile-negative mononucleosis.
  • Differ from EBV?
  • Fever and malaise often persist for more than 2
    weeks.
  • The expected outcome is complete recovery.
  • Rare complications peripheral neuropathy,
    hemolytic anemia, thrombocytopenia, pneumonia,
    retinitis, gastrointestinal ulceration and
    encephalitis.

13
Congenital CMV infection
  • More than 90 of children have no clinical
    evidence of disease as newborns.
  • Lab abnormalities reflect involvement of
    hepatobiliary , hematopoeitic and CNS.
  • Newborns with symptomatic infection have wide
    range of severity.
  • Mortality is 10-15
  • Among symptomatic survivors, neonatal clinical
    abnormalities can be expected to resolve within
    weeks except for those involving CNS and hearing.

14
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15
Outcome
  • Mental retardation.
  • Hearing loss 7-15 in initially asymptomatic
    newborn
  • Cerebral palsy.
  • Retinal damage.

16
Congenital CMV infection
  • Factors associated with increased risk of CNS
    sequel
  • Primary maternal infection during pregnancy.
  • Abnormal neurologic examination findings.
  • Microcephaly.
  • Brain C.T.scan abnormalities.
  • Increased CSF protein.
  • Chorioretinitis.

17
Perinatal/Neonatal CMV infection
  • It is not associated with newborn illness or CNS
    sequel, except perhaps in very preterm newborns
    who have very low levels of passively acquired
    antibody at the time of infection and they may be
    left with residual neurologic sequelae
    psychomotor retardation.
  • It is not associated with increase hearing loss,
    chorioretinitis or microcephaly.
  • Transfusion acquired CMV to newborns whose
    mothers are seronegative can cause a picture
    similar to congenital infection and presents with
    jaundice, hepatosplenomegaly, abnormal liver
    function, thrombocytopenia, hearing loss and
    pulmonary problems.

18
Differential diagnosis in the newborn
  • TORCHS.
  • Acute viral ,bacterial or systemic fungal
    infections.
  • In born errors of metabolism can cause neonatal
    hepatitis,thrombocytopenia , hepatosplenomegaly ,
    encephalopathy and anemia.

19
CMV in Immunocompromised children
  • The majority are due to reactivation of the host
    CMV and these often are clinically silent.
  • When primary infection occurs by blood products
    and transplanted organ, it is usually associated
    with disease.
  • The clinical manifestation correlates with the
    degree of immunologic impairment.
  • Primary CMV infection in transplant patients
    frequently is heralded by fever and leucopoenia,
    rash, arthralgia and elevated serum alanine
    aminotransferase levels.

20
CMV in Immunocompromised children
  • Complications in transplant patients
  • Impaired function of the transplanted organ.
  • Pneumonitis, G.I. Ulceration, hepatitis.
  • Opportunistic fungal infection.

21
CMV in Immunocompromised children
  • Complications in AIDS patients
  • Retinitis.
  • Esophagitis , Colitis , Hepatitis.
  • Encephalitis,peripheral neuropathy.
  • Pneumonitis.
  • Treatment is palliative requiring therapy with
    Ganciclovir, Foscarnet or Cidofovir followed by
    maintenance therapy with one of these drugs which
    is continued indefinitely or until the patient
    immune function improves and stabilizes.

22
Laboratory diagnosis
  • Congenital CMV infection is diagnosed by
  • Detection of virus in the urine or saliva of a
    newborn
  • PCR.
  • CMV IgM transient.
  • Detection of CMV within the first 3 weeks of life
    is considered proof of congenital CMV but after
    this period it is not certain if it is due to
    prenatal or perinatal infection.
  • Viremia demonstrated by buffy coat or DNA
    indicates active infection.

23
Laboratory diagnosis
  • Diagnosis of CMV infections in immunocompromised
    patients is much more difficult.
  • Serology is of limited value.
  • CMV IgG is a good marker for past infection and
    identifies the problematic positive
    donor/negative recipient situation that carries a
    high risk for primary infection and CMV disease
    in the immediate post transplant period.

24
Laboratory diagnosis
  • Detection of CMV in blood is a much better
    predictor of disease among immunocompromised
    patients than is shedding of virus.
  • Quantitative tests has good correlation with the
    clinical picture either by detection of WBC
    positive for CMV antigens by immunofluorescence
    or quantitative PCR.

25
Laboratory diagnosis
  • Congenital infection
  • Virus isolation.
  • IgG
  • IgM

26
Management
  • Antiviral treatment has reduced the burden of
    CMV disease substantially in immunocompromised
    patients.
  • Ganciclovir, Foscarnet, and Cidofovir.
  • No antiviral agent is approved for treatment of
    congenital CMV infection but.
  • Side effects include neutropenia ,
    thrombocytopenia , liver dysfunction
    ,reproductive toxicity and carcinogenicity.

27
Management
  • The approach to antiviral treatment in
    immunocompromised patients can vary with
  • The clinical settings.
  • The type of CMV infection.
  • Clinical manifestations of CMV disease.
  • Laboratory evidence of CMV infection.
  • Degree of immunosuppression.

28
Anticipatory management
29
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30
Prevention
  • All preschool-age children should be considered
    potential sources of infection.
  • Avoid contact with body fluids from young
    children and careful hand washing
  • Educating women before getting pregnant.
  • Vaccination.
  • Limit transfusion-acquired CMV infection.
  • Prophylactic antiviral treatment and passive
    immunization to prevent CMV disease after
    transplantation.

31
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