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PEDIATRICS Vol. 104 No. 2 August 1999, p. e14
Received Nov 9, 1998; accepted Mar 23, 1999.
,
, ¶, #,,,, ¶, #, and
From the * Department of Pediatrics, Division of
Pediatric Cardiology, Presbyterian Hospital/Columbia University School
of Medicine, New York, New York; the Department of Cardiology,
Children's Hospital, Boston, Massachusetts; the § Department of
Pediatrics, Division of Pediatric Cardiology, University of California,
Los Angeles Medical Center and School of Medicine, Los Angeles,
California; the Departments of Biostatistics and ¶ Epidemiology and
# Pediatrics, ** Division of Pediatric Cardiology, Cleveland Clinic,
Cleveland, Ohio; the Department of Pediatrics, Division of
Pediatric Cardiology, Baylor College of Medicine, Houston, Texas; the
§§ National Institutes of Health, National Heart, Lung and Blood
Institute, Bethesda, Maryland; and the || Department of Pediatrics,
Division of Pediatric Cardiology, Mt Sinai School of Medicine, New
York, New York.
Objective. Although numerous cardiac abnormalities have been reported in HIV-infected children, precise estimates of the incidence of cardiac disease in these children are not well-known. The objective of this report is to describe the 2-year cumulative incidence of cardiac abnormalities in HIV-infected children.
Methodology: Design. Prospective cohort (Group I) and inception cohort (Group II) study design.
Setting. A volunteer sample from 10 university and public hospitals.
Participants. Group I consisted of 205 HIV vertically infected children enrolled at a median age of 22 months. This group was comprised of infants and children already known to be HIV-infected at the time of enrollment in the study. Most of the children were African-American or Hispanic and 89% had symptomatic HIV infection at enrollment. The second group included 611 neonates born to HIV-infected mothers, enrolled during fetal life or before 28 days of age (Group II). In contrast to the older Group I children, all the Group II children were enrolled before their HIV status was ascertained.
Interventions. According to the study protocol, children underwent a series of cardiac evaluations including two-dimensional echocardiogram and Doppler studies of cardiac function every 4 to 6 months. They also had a 12- or 15-lead surface electrocardiogram (ECG), 24-hour ambulatory ECG monitoring, and a chest radiograph every 12 months.
Outcome Measures. Main outcome measures were the
cumulative incidence of an initial episode of left ventricular (LV)
dysfunction, cardiac enlargement, and congestive heart failure
(CHF). Because cardiac abnormalities tended to cluster in the
same patients, we also determined the number of children who had
cardiac impairment which we defined as having either left
ventricular fractional shortening (LV FS) 
25% after 6 months
of age, CHF, or treatment with cardiac medications.
Results: Cardiac Abnormalities. In Group I
children (older cohort), the prevalence of decreased LV function (FS
25%) was 5.7% and the 2-year cumulative incidence (excluding
prevalent cases) was 15.3%. The prevalence of echocardiographic LV
enlargement (LV end-diastolic dimension z score >2) at
the time of the first echocardiogram was 8.3%. The cumulative
incidence of LV end-diastolic enlargement was 11.7% after 2 years.The cumulative incidence of CHF and/or the use of cardiac
medications was 10.0% in Group I children. There were 14 prevalent cases of cardiac impairment (LV FS 25% after 6 months of age, CHF,
or treatment with cardiac medications) in Group I. After excluding
these prevalent cases, the 2-year cumulative incidence of cardiac
impairment was 19.1% among Group I children and 80.9% remained free
of cardiac impairment after 2 years of follow-up. Within Group II (neonatal cohort), the 2-year cumulative incidence of
decreased LV FS was 10.7% in the HIV-infected children compared
with 3.1% in the HIV-uninfected children. LV dilatation was
also more common in Group II infected versus uninfected children (8.7%
vs 2.1%). The cumulative incidence of CHF and/or the use of cardiac
medications was 8.8% in Group II infected versus 0.5% in uninfected
subjects. The 1- and 2-year cumulative incidence rates of cardiac
impairment for Group II infected children were 10.1% and 12.8%,
respectively, with 87.2% free of cardiac impairment after the first 2 years of life.
Mortality. In the Group I cohort, the 2-year cumulative death rate from all causes was 16.9% [95% CI: 11.7%-22.1%]. The 1- and 2-year mortality rates after the diagnosis of CHF (Kaplan-Meier estimates) were 69% and 100%, respectively. In the Group II cohort, the 2-year cumulative death rate from all causes was 16.3% [95% CI: 8.8%-23.9%] in the HIV-infected children compared with no deaths among the 463 uninfected Group II children. Two of the 4 Group II children with CHF died during the 2-year observation period and 1 more died within 2 years of the diagnosis of CHF. The 2-year mortality rate after the diagnosis of CHF was 75%.
Conclusions. This study reports that in addition to subclinical cardiac abnormalities previously reported by the P2C2 Study Group, an important number of HIV-infected children develop clinical heart disease. Over a 2-year period, approximately 10% of HIV-infected children had CHF or were treated with cardiac medications. In addition, approximately 20% of HIV-infected children developed depressed LV function or LV dilatation and it is likely that these abnormalities are hallmarks of future clinically important cardiac dysfunction. Cardiac abnormalities were found in both the older (Group I) as well as the neonatal cohort (Group II) (whose HIV infection status was unknown before enrollment) thereby minimizing potential selection bias based on previously known heart disease.Based on these findings, we recommend that clinicians need to maintain a high degree of suspicion for heart disease in HIV-infected children. All HIV-infected infants and children should have a thorough baseline cardiac evaluation. Patients who develop symptoms of heart or lung disease should undergo more detailed cardiac examinations including ECG and cardiac ultrasound. Key words: HIV, cardiac disease, pediatrics.
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