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Abstract
A metaanalysis of surfactant clinical trials was carried out to assess whether or
not an association exists between exogenous surfactant therapy and pulmonary hemorrhage.
Trials that reported the pulmonary hemorrhage occurrence (group 1) and those that
did not (group 2) were analyzed. Thirty-three treatment strategies were tested in
29 publications from 1980 through 1992. Eleven of these were group 1 trials, which
reported a 3% overall incidence of pulmonary hemorrhage. The rates were significantly
higher in both the treated and the control groups of natural surfactant trials than
in synthetic surfactant trails (5.87% and 5.36% in the natural surfactant trials vs
2.51% and 1.04% in the synthetic surfactant trials, respectively). The pooled estimate
of relative risk for pulmonary hemorrhage with any surfactant therapy was 1.47 (95%
confidence interval 1.05, 2.07; p < 0.05). Logistic regression modeling revealed that
the nature of surfactant, treatment strategy, and lower mean birth weight had a significant
influence on the relative risk of pulmonary hemorrhage; a similar trend was seen with
higher mortality rates. Variation in the rates of patent ductus arteriosus did not
have an independent effect on the estimated pulmonary hemorrhage risk. Most group
2 trials were published before 1990, and the median total sample size was 73, compared
with 402 for the group 1 trials (p < 0.05), most of which were published in the 1990s.
In 10 (50%) of 20 group 2 trials, pulmonary hemorrhage data were collected methodically,
in comparison with all group 1 trials, most of which collected data prospectively.
We conclude that pulmonary hemorrhage is a rare complication of respiratory distress
syndrome. An awareness of the possible association of pulmonary hemorrhage with surfactant
use in later trials and the differences in definitions and reporting practices probably
explain variations in the reported incidence among the trials. The risk of pulmonary
hemorrhage increases slightly, on an average of 47%, with any surfactant therapy.
This increased risk is small compared with the documented benefits of surfactant therapy
in respiratory distress syndrome.