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Clinical and Diagnostic Laboratory Immunology, July 1999, p. 464-470, Vol. 6, No. 4
Dana Farber Cancer Institute and Harvard
University Medical School, Boston, Massachusetts 02115
Received 19 October 1998/Returned for modification 10 February
1999/Accepted 18 March 1999
Pertussis in infants is often severe, resulting in prolonged
hospitalization. Treatment is limited to supportive care. Antibiotics do not significantly alter the course of the disease unless
administered during the catarrhal phase. Therapies directed at
pertussis toxin, a major virulence factor of Bordetella
pertussis, may be beneficial. This study uses the aerosol
challenge model to further examine the protective effects of P-IGIV, a
new intravenous immunoglobulin product, which has high levels of
pertussis toxin antibodies. P-IGIV was prepared as a 4% immunoglobulin
G (IgG) solution from the pooled donor plasma from donors immunized
with inactivated pertussis toxoid. The IgG pertussis toxin antibody
concentration in P-IGIV is >7-fold higher than conventional
intravenous immunoglobulin products. In the aerosol challenge model,
P-IGIV-treated mice exhibited a dose-dependent decrease in mortality
when monitored for 28 days postchallenge. P-IGIV in doses of 2,800, 1,400, and 350 mg/kg significantly reduced mortality compared to saline
(P < 0.01)- and human IGIV (P < 0.01)-treated controls. The 50% protective dose of pertussis toxin
antibodies in P-IGIV was 147 µg/ml. Recovery of weight gain and
normalization of leukocyte counts occurred in all P-IGIV-treated groups
but did not exhibit dose-dependent characteristics. Even after 7 days
of infection, P-IGIV reversed the effects of pertussis in mice. This
study provides further evidence that pertussis toxin antibodies not
only play a role in passive protection but can also reverse symptoms of
established disease in mice. We feel that P-IGIV deserves further
evaluation in children hospitalized with severe pertussis.
1071-412X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
Protective Effects of Pertussis Immunoglobulin
(P-IGIV) in the Aerosol Challenge Model
*
Corresponding author. Mailing address: Pharmacia & Upjohn, 9156-243-131, 7000 Portage Rd., Kalamazoo, MI 49001. Phone:
(616) 833-8714. Fax: (616) 833-0203. E-mail: jbbruss{at}am.pnu.com.
Present address: Wyeth-Lederle Vaccines, Pearl River, N.Y.
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