AI Article Synopsis
- Despite the rise in pertussis rates globally despite vaccination efforts, no specific treatments are available, leading to significant infant health issues.
- Humanized monoclonal antibodies that neutralize the pertussis toxin were developed and tested, showing promise in reducing white blood cell counts and bacterial colonization in mice.
- The antibodies also demonstrated effectiveness in baboons by reducing white blood cell increases and enhancing bacterial clearance, suggesting potential for treating neonatal pertussis in humans alongside standard care methods.
Article Abstract
Despite widespread vaccination, pertussis rates are rising in industrialized countries and remain high worldwide. With no specific therapeutics to treat disease, pertussis continues to cause considerable infant morbidity and mortality. The pertussis toxin is a major contributor to disease, responsible for local and systemic effects including leukocytosis and immunosuppression. We humanized two murine monoclonal antibodies that neutralize pertussis toxin and expressed them as human immunoglobulin G1 molecules with no loss of affinity or in vitro neutralization activity. When administered prophylactically to mice as a binary cocktail, antibody treatment completely mitigated the Bordetella pertussis-induced rise in white blood cell counts and decreased bacterial colonization. When administered therapeutically to baboons, antibody-treated, but not untreated control animals, experienced a blunted rise in white blood cell counts and accelerated bacterial clearance rates. These preliminary findings support further investigation into the use of these antibodies to treat human neonatal pertussis in conjunction with antibiotics and supportive care.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5075433 | PMC |
| http://dx.doi.org/10.1126/scitranslmed.aad0966 | DOI Listing |
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