ROLE OF FETAL ECHOCARDIOGRAPHY IN CONGENITAL HEART DISEASES - PowerPoint PPT Presentation

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ROLE OF FETAL ECHOCARDIOGRAPHY IN CONGENITAL HEART DISEASES

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Title: ROLE OF FETAL ECHOCARDIOGRAPHY IN CONGENITAL HEART DISEASES


1
ROLE OF FETAL ECHOCARDIOGRAPHY IN CONGENITAL
HEART DISEASES
  • BY JAMEEL A. AL-ATA CONSULTANT AND ASSISTANT
    PROFESSOR OF PEDIATRIC CARDIOLOGY

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INTRODUCTION
  • Incidence of CHD is 6-8/1000 live births and
    about 1.5 in the fetus population.
  • Nearly all types of postnatally diagnosed CHD
    types were diagnosed prenatally.
  • The more complex in utero CHD the more diagnosed
    and the simpler can be missed in utero (ASD, mild
    AS, mild PS).
  • Some CHD types are shown to evolve and progress
    in utero e.g Valvar AS.
  • 17-48 of in utero CHD is associated with
    chromosomal abnormalities (only 5-10
    postnatally) and 20 with extracardiac
    malformations.

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INTRODUCTION, CONT
  • Fetal Echocardiography is an accurate diagnostic
    tool for CHD (85-90 sensitivity 99
    specificity) when using state of the art U/S
    technology and when pediatric cardiology/fetal
    medicine collaborates.
  • Routine obstetrical U/S is not a good screening
    test for CHD. It is both late (20-24 wks) and
    not comprehensive.
  • Indications include DM, INFESTIONS, TERATOGENS
    ABN 4 CH VIEW, HX OF CHILD WITH CHD, CHROMOSOMAL
    ABN, EXT CARDIAC ABN, DEXTROCARDIA, SITUS
    INVERSUS, FETAL GROWTH RETARDATION AND FETAL
    ARRHYTHMIA.

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Fig. 5 Apical four chamber view of the fetal
heart (LV, left ventricle RV, right ventricle
LA, left atrium RA, right atrium MB moderator
band PV, pulmonary veins Ao, descending aorta
S, fetal spine)
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IMPACT OF FETAL ECHOCARDIOGRAPHY
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ON EPIDEMIOLOGY
  • Malformations due to pregnancy termination True
    incidence of CHD is 1.0 (0.2-0.4 higher than
    detected postnatally).
  • Up to 48 of in utero CHD is associated with
    chromosomal anomalies and 20 with extracardiac
    malformations.
  • Possible decreased prevalence of subsets of CHD
    associated with severe extracardiac malformations.

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continue
  • In a recent study
  • one hundred and forty-nine fetuses with CHD and
    normal karyotype were analyzed. Seventy-six
    fetuses had conotruncal anomalies.
  • 22q11.2 deletion was present in 10 cases (6.7),
    all of which had conotruncal anomalies (13.1).

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continue
  • Thymic hypoplasia or absence was suspected in 11
    cases with conotruncal anomaly. Nine of these 11
    had the deletion two cases were false positive.
  • One fetus with a normal-sized thymus had
    deletion of 22q11.2 (sensitivity 90, specificity
    98.5, positive predictive value 81.8, and
    negative predictive value 99.2).

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ON FETAL NEONATAL WELL-BEING
  • Timed delivery in tertiary care centers.
  • Decreased morbidity and perhaps better long term
    outcome of infants with semi lunar valves
    obstruction and/or ductal dependant lesions.
  • Intrauterine treatment (e.g. fetal arrhythmias).
  • Monitoring fetal well being during maternal
    trearment

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ON MANAGEMENT
  • Better prognostication and counseling.
  • Pregnancy termination at the appropriate time.
  • Better understanding of the pathophysiology and
    evolution of CHD.

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HOW TO GET A REAL IMPACT
  • Fetal echocardiographic screening at 11-14 weeks
    of gestation.
  • Screening of both low risk and high risk
    pregnancies.
  • Developing markers.
  • Collaboration and the use of state of art U/S
    with Doppler, color flow Doppler and power
    Doppler..etc.

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Continuation
  • Including the ventricular outflow tracts with the
    four chamber view in obstetrical U/S.
  • Training obstetrical technicians to do so.
  • Developing safe intra uterine interventional
    procedures.

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CONCLUSION
  • Fetal echocardiography main impact is on
    incidence and appropriate prenatal, perinatal
    treatment.
  • It is a demanding, yet, promising tool.
  • Sequential studies are needed to track evolving
    lesions.
  • Limitations include operator level of expertise,
    technology, nature of CHD, number of
    collaborating centers, level of awareness and
    referralsetc.

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  • a family history of congenital heart disease
  • an abnormal fetal heart rhythm
  • fetal heart abnormalities detected during a
    routine pregnancy ultrasound scan
  • abnormality of another major organ system
  • insulin-dependent (type 1) diabetes mellitus
  • exposure to some drugs in early pregnancy. For
    example, some anti-epileptic drugs can damage the
    developing heart.
  • abnormal amniocentesis (AM'ne-o-sen-TE'sis). This
    is abnormal amniotic fluid in the woman's uterus.

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THANK YOU
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  • Maternal Drug Exposure and Diseases
  • Women with seizure disorders taking
    anti-convulsantsWomen taking lithium for
    depressionWomen taking insulin for
    diabetesWomen who have phenylketonuriaWomen
    exposed to Rubella
  • Family History of Congenital Heart Disease
  • Previous child with CHD, new risk is 1 in 20 to 1
    in 100Previous two children with CHD, new risk
    is 1 in 10 to 1 in 20Mother has CHD, new risk is
    as high as 1 in 5 to 1 in 20Father has CHD, new
    risk 1 in 30
  • Increased Maternal Risk for Down Syndrome and
    Other Chromosomal Defects

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  • Chromosome abnormalities and CHD
  • Down syndrome
  • Trisomy 18 and Trisomy 13
  • Turner's syndrome
  • Cri du chat syndrome
  • Wolf-Hirshhorn syndrome
  • DiGeorge syndrome (deletion 22q11)
  • Ultrasound -Identified Fetal Birth Defects of the
    Current Pregnancy

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  • Other Rare Genetic Diseases
  • Marfan syndrome
  • Smith-Lemli-Opitz syndrome
  • Ellis-van Creveld
  • Holt-Oram syndrome
  • Noonan syndrome
  • Mucopolysaccharidoses
  • Goldenhar syndrome (hemifacial microsomia)
  • William's syndrome
  • VACTERL association (tracheal and esophageal
    malformations associated with vertebral,
    anorectal, cardiac, renal, radial, and limb
    abnormalities).
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