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Antimicrobial Agents and Chemotherapy, May 1999, p. 1183-1188, Vol. 43, No. 5
Department of Pediatrics, New England Medical
Center, Tufts University School of Medicine, Boston, Massachusetts
021111; Ross Products Division,
Columbus, Ohio 432152; Department of
Pediatrics, National Children's Medical Center, Washington, D.C.
200103; Department of Pediatrics,
Children's Hospital of Buffalo, Buffalo, New York
422224; Royal Children's Hospital,
Received 1 June 1998/Returned for modification 5 September
1998/Accepted 25 February 1999
We conducted a multicenter, double-blind, placebo-controlled,
randomized trial of a humanized monoclonal antibody against a
respiratory syncytial virus (RSV) fusion protein (SB 209763) to
evaluate its safety, pharmacokinetics, and fusion inhibition and
neutralization titers. Forty-three infants who were either delivered
prematurely (
0066-4804/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
Safety and Pharmacokinetics of an Intramuscular
Monoclonal Antibody (SB 209763) against Respiratory Syncytial Virus
(RSV) in Infants and Young Children at Risk for Severe RSV
Disease
35 weeks' gestation) or exhibited bronchopulmonary dysplasia were administered either single or repeat (two doses, 8 weeks
apart) intramuscular injections of SB 209763 at a concentration of
0.25, 1.25, 5.0, or 10.0 mg/kg or of a placebo. Four of 229 adverse
events were considered related to the study drug, including purpura
(n = 3) and thrombocytosis (n = 1).
No subject developed a detectable level of anti-SB 209763 antibody.
Approximately 1 week after administration of the second dose of SB
209763 at 10 mg/kg, the mean plasma concentration (n = 9) was 68.5 µg/ml. The terminal half-life
(T1/2) determined by noncompartmental analysis ranged from 22 to 50 days. The population pharmacokinetics for SB
209763 following intramuscular administration was appropriately described by a one-compartment model with first-order input and elimination. Higher values for clearance and volume of distribution at
steady state were observed for younger patients, with values decreasing
to 0.143 (ml/h)/kg and 161 mL/kg, respectively, by a mean age of 298 days (~10 months). The mean T1/2 of SB 209763 for the study population was 32.5 days. No other factor (dose, weight,
gender, race, premature birth, or bronchopulmonary dysplasia) was
observed to alter the population pharmacokinetics of SB 209763 in this
study of infants and young children. The mean neutralization titer on
day 6 was 286, and the mean fusion inhibition titer was 36. At least
57% of subjects dosed at 1.25 to 10.0 mg of SB 209763 per kg of body
weight who were seronegative at baseline experienced a fourfold or
greater increase in fusion inhibition titer. Nine RSV infections were
documented during the 16-week course of the study; the numbers of RSV
infections were similar for the different regimens, including the
placebo. The doses of SB 209763 studied may have been insufficient to
confer protection against RSV lower respiratory tract disease; these
results suggest that additional trials using higher doses of monoclonal
antibody for immunoprophylaxis should be considered.
*
Corresponding author. Mailing address: New England
Medical Center, Box 321, 750 Washington St., Boston, MA 02111. Phone:
(617) 636-5227. Fax: (617) 636-4300. E-mail:
cmeissner{at}es.nemc.org.
Present address: Hawthorne Research and Consulting, King of
Prussia, PA 19406.
| Clin. Vaccine Immunol. | Clin. Microbiol. Rev. |
|---|---|
| J. Clin. Microbiol. | ALL ASM JOURNALS |
