Treatment of Severe Pertussis: a Study of the Safety and Pharmacology of Intravenous Pertussis Immunoglobulin

Overview

Journal Pediatr Infect Dis J

Specialty Pediatrics

Date 1999 Jul 3

PMID 10391179

Citations 21

Authors

J B Bruss

R Malley

S Halperin

S Dobson

M Dhalla

J McIver

G R Siber

Affiliations

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Abstract

Background: Pertussis in infants is often severe, resulting in complications and prolonged hospitalization. Treatment is limited to supportive care. Antibiotics do not significantly alter the course of the disease. Therapies directed at pertussis toxin, a major virulence factor of Bordetella pertussis, might be beneficial. This study examines the safety and pharmacology of intravenous pertussis immunoglobulin (P-IGIV), which has high levels of pertussis toxin antibodies.

Methods: P-IGIV was prepared as a 4% IgG solution from the pooled plasma from donors immunized with inactivated pertussis toxoid. The IgG pertussis toxin antibody concentration of 733 microg/ml is >7-fold higher than contained in conventional intravenous immunoglobulin products. Children with presumptive pertussis were allocated to one of three treatment doses of P-IGIV.

Results: Twenty-six of 30 enrolled children had confirmed pertussis. There were no adverse events associated with P-IGIV except one patient who had transient hypotension that responded to an infusion rate decrease. P-IGIV doses of 1500, 750 and 250 mg/kg achieved > or =4-fold, 3-fold and >2-fold rises in peak geometric mean titers of pertussis toxin IgG antibodies, respectively. P-IGIV exhibited a half-life of 38.4 days and a volume of distribution of 87.8 ml/kg. All three treatment groups showed declines in lymphocytosis (P < 0.05) and paroxysmal coughing by the third day after P-IGIV infusion compared with preinfusion values.

Conclusion: P-IGIV is safe and achieves high pertussis toxin antibody titers in infants. This study provides data for a prospective, controlled trial of P-IGIV.

Citing Articles

Plasma therapy: a passive resistance against the deadliest.

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Neutralization of pertussis toxin by a single antibody prevents clinical pertussis in neonatal baboons.

Nguyen A, DiVenere A, Papin J, Connelly S, Kaleko M, Maynard J Sci Adv. 2020; 6(6):eaay9258.

PMID: 32076653 PMC: 7002138. DOI: 10.1126/sciadv.aay9258.

Pertussis Toxin: A Key Component in Pertussis Vaccines?.

Gregg K, Merkel T Toxins (Basel). 2019; 11(10).

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Role of Major Toxin Virulence Factors in Pertussis Infection and Disease Pathogenesis.

Scanlon K, Skerry C, Carbonetti N Adv Exp Med Biol. 2019; 1183:35-51.

PMID: 31376138 PMC: 7038575. DOI: 10.1007/5584_2019_403.

Association of Pertussis Toxin with Severe Pertussis Disease.

Scanlon K, Skerry C, Carbonetti N Toxins (Basel). 2019; 11(7).

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