A1,
A2,
B,
C1,
C2,
D,
E,
F,
G-H,
I-K,
L,
M,
N,
O,
P1,
P2,
Q-R,
S,
T,
U-V,
W-Z
Survanta Side Effects, and Drug Interactions - Beractant
Survanta Side Effects, and Drug Interactions - Beractant
SIDE EFFECTS
The most commonly reported adverse experiences were associated with the dosing
procedure. In the multiple-dose controlled clinical trials, each dose of SURVANTA
was divided into four quarter-doses which were instilled through a catheter
inserted into the endotracheal tube by briefly disconnecting the endotracheal
tube from the ventilator. Transient bradycardia occurred with 11.9% of doses.
Oxygen desaturation occurred with 9.8% of doses.
Other reactions during the dosing procedure occurred with fewer than 1% of
doses and included endotracheal tube reflux, pallor, vasoconstriction, hypotension,
endotracheal tube blockage, hypertension, hypocarbia, hypercarbia, and apnea.
No deaths occurred during the dosing procedure, and all reactions resolved with
symptomatic treatment.
The occurrence of concurrent illnesses common in premature infants was evaluated
in the controlled trials. The rates in all controlled studies are in Table 3.
TABLE 3
|
|
All Controlled Studies |
|
|
SURVANTA |
Control |
|
|
Concurrent Event
|
(%) |
(%) |
P- Value a |
|
Patent ductus arteriosus
|
46.9 |
47.1 |
0.814 |
|
Intracranial hemorrhage
|
48.1 |
45.2 |
0.241 |
|
Severe intracranial hemorrhage
|
24.1 |
23.3 |
0.693 |
|
Pulmonary air leaks
|
10.9 |
24.7 |
<0.001 |
|
Pulmonary interstitial emphysema
|
20.2 |
38.4 |
<0.001 |
|
Necrotizing enterocolitis
|
6.1 |
5.3 |
0.427 |
|
Apnea
|
65.4 |
59.6 |
0.283 |
|
Severe apnea
|
46.1 |
42.5 |
0.114 |
|
Post-treatment sepsis
|
20.7 |
16.1 |
0.019 |
|
Post-treatment infection
|
10.2 |
9.1 |
0.345 |
|
Pulmonary hemorrhage
|
7.2 |
5.3 |
0.166 |
|
a P -value comparing groups in controlled
studies
|
When all controlled studies were pooled, there was no difference in intracranial
hemorrhage. However, in one of the single-dose rescue studies and one of the
multiple-dose prevention studies, the rate of intracranial hemorrhage was significantly
higher in SURVANTA patients than control patients (63.3% v 30.8%, P
=0.001; and 48.8% v 34.2%, P =0.047, respectively). The rate
in a Treatment IND involving approximately 8100 infants was lower than in the
controlled trials.
In the controlled clinical trials, there was no effect of SURVANTA on results
of common laboratory tests: white blood cell count and serum sodium, potassium,
bilirubin, creatinine.
More than 4300 pretreatment and posttreatment serum samples from approximately
1500 patients were tested by Western Blot Immunoassay for antibodies to surfactant-associated
proteins SP-B and SP-C. No IgG or IgM antibodies were detected.
Several other complications are known to occur in premature infants. The following
conditions were reported in the controlled clinical studies. The rates of the
complications were not different in treated and control infants, and none of
the complications were attributed to SURVANTA.
Respiratory: lung consolidation, blood from the endotracheal tube, deterioration
after weaning, respiratory decompensation, subglottic stenosis, paralyzed diaphragm,
respiratory failure.
Cardiovascular: hypotension, hypertension, tachycardia, ventricular
tachycardia, aortic thrombosis, cardiac failure, cardio-respiratory arrest,
increased apical pulse, persistent fetal circulation, air embolism, total anomalous
pulmonary venous return.
Gastrointestinal: abdominal distention, hemorrhage, intestinal perforations,
volvulus, bowel infarct, feeding intolerance, hepatic failure, stress ulcer.
Renal: renal failure, hematuria.
Hematologic: coagulopathy, thrombocytopenia, disseminated intravascular
coagulation.
Central Nervous System: seizures.
Endocrine/Metabolic: adrenal hemorrhage, inappropriate ADH secretion,
hyperphosphatemia.
Musculoskeletal: inguinal hernia.
Systemic: fever, deterioration.
Follow-Up Evaluations
To date, no long-term complications or sequelae of SURVANTA therapy have been
found.
Single-Dose Studies
Six-month adjusted-age follow-up evaluations of 232 infants (115 treated) demonstrated
no clinically important differences between treatment groups in pulmonary and
neurologic sequelae, incidence or severity of retinopathy of prematurity, rehospitalizations,
growth, or allergic manifestations.
Multiple-Dose Studies
Six-month adjusted age follow-up evaluations have been completed in 631 (345
treated) of 916 surviving infants. There were significantly less cerebral palsy
and need for supplemental oxygen in SURVANTA infants than controls. Wheezing
at the time of examination was significantly more frequent among SURVANTA infants,
although there was no difference in bronchodilator therapy.
Final twelve-month follow-up data from the multiple-dose studies are available
from 521 (272 treated) of 909 surviving infants. There was significantly less
wheezing in SURVANTA infants than controls, in contrast to the six-month results.
There was no difference in the incidence of cerebral palsy at twelve months.
Twenty-four month adjusted age evaluations were completed in 429 (226 treated)
of 906 surviving infants. There were significantly fewer SURVANTA infants with
rhonchi, wheezing, and tachypnea at the time of examination. No other differences
were found.
DRUG INTERACTIONS
No Information Provided.
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